Planet Neuroscience

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Median nerve stimulation based BCI: a new approach to detect intraoperative awareness during general anesthesia

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on June 19, 2019 04:25 AM.

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Inferred successor maps for better transfer learning. (arXiv:1906.07663v1 [cs.AI])

Humans and animals show remarkable flexibility in adjusting their behaviour when their goals, or rewards in the environment change. While such flexibility is a hallmark of intelligent behaviour, these multi-task scenarios remain an important challenge for machine learning algorithms and neurobiological models alike. Factored representations can enable flexible behaviour by abstracting away general aspects of a task from those prone to change, while nonparametric methods provide a principled way of using similarity to past experiences to guide current behaviour. Here we combine the successor representation (SR), that factors the value of actions into expected outcomes and corresponding rewards, with evaluating task similarity through nonparametric inference and clustering the space of rewards. The proposed algorithm improves SR's transfer capabilities by inverting a generative model over tasks, while also explaining important neurobiological signatures of place cell representation in the hippocampus. It dynamically samples from a flexible number of distinct SR maps while accumulating evidence about the current reward context, and outperforms competing algorithms in settings with both known and unsignalled rewards changes. It reproduces the "flickering" behaviour of hippocampal maps seen when rodents navigate to changing reward locations, and gives a quantitative account of trajectory-dependent hippocampal representations (so-called splitter cells) and their dynamics. We thus provide a novel algorithmic approach for multi-task learning, as well as a common normative framework that links together these different characteristics of the brain's spatial representation.

in q-bio.NC updates on arXiv.org on June 19, 2019 01:30 AM.

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Quantized Three-Ion-Channel Neuron Model for Neural Action Potentials. (arXiv:1906.07570v1 [q-bio.NC])

The Hodgkin-Huxley model describes the conduction of the nervous impulse through the axon, whose membrane's electric response can be described employing multiple connected electric circuits containing capacitors, voltage sources, and conductances. These conductances depend on previous depolarizing membrane voltages, which can be identified with a memory resistive element called memristor. Inspired by the recent quantization of the memristor, a simplified Hodgkin-Huxley model including a single ion channel has been studied in the quantum regime. Here, we study the quantization of the complete Hodgkin-Huxley model, accounting for all three ion channels, and introduce a quantum source, together with an output waveguide as the connection to a subsequent neuron. Our system consists of two memristors and one resistor, describing potassium, sodium, and chloride ion channel conductances, respectively, and a capacitor to account for the axon's membrane capacitance. We study the behavior of both ion channel conductivities and the circuit voltage, and we compare the results with those of the single channel, for a given quantum state of the source. It is remarkable that, in opposition to the single-channel model, we are able to reproduce the voltage spike in an adiabatic regime. Arguing that the circuit voltage is a quantum variable, we find a purely quantum-mechanical contribution in the system voltage's second moment. This work represents a complete study of the Hodgkin-Huxley model in the quantum regime, establishing a recipe for constructing quantum neuron networks with quantum state inputs. This paves the way for advances in hardware-based neuromorphic quantum computing, as well as quantum machine learning, which might be more efficient resource-wise.

in q-bio.NC updates on arXiv.org on June 19, 2019 01:30 AM.

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Core language brain network for fMRI-language task used in clinical applications. (arXiv:1906.07546v1 [q-bio.NC])

Functional magnetic resonance imaging (fMRI) is widely used in clinical applications to highlight brain areas involved in specific cognitive processes. Brain impairments, such as tumors, suppress the fMRI activation of the anatomical areas they invade and, thus, brain-damaged functional networks present missing links/areas of activation. The identification of the missing circuitry components is of crucial importance to estimate the damage extent. The study of functional networks associated to clinical tasks but performed by healthy individuals becomes, therefore, of paramount concern. These `healthy' networks can, indeed, be used as control networks for clinical studies.In this work we investigate the functional architecture of 20 healthy individuals performing a language task designed for clinical purposes. We unveil a common architecture persistent across all subjects under study, which involves Broca's area, Wernicke's area, the Premotor area, and the pre-Supplementary motor area. We study the connectivity weight of this circuitry by using the k-core centrality measure and we find that three of these areas belong to the most robust structure of the functional language network for the specific task under study. Our results provide useful insight for clinical applications on primarily important functional connections which, thus, should be preserved through brain surgery.

in q-bio.NC updates on arXiv.org on June 19, 2019 01:30 AM.

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ADAM30 Downregulates APP-Linked Defects Through Cathepsin D Activation in Alzheimer's Disease. (arXiv:1906.07511v1 [q-bio.NC])

Although several ADAMs (A disintegrin-like and metalloproteases) have been shown to contribute to the amy-loid precursor protein (APP) metabolism, the full spectrum of metalloproteases involved in this metabolism remains to be established. Transcriptomic analyses centred on metalloprotease genes unraveled a 50% decrease in ADAM30 expression that inversely correlates with amyloid load in Alzheimer's disease brains. Accordingly, in vitro down-or up-regulation of ADAM30 expression triggered an increase/decrease in A$\beta$ peptides levels whereas expression of a biologically inactive ADAM30 (ADAM30 mut) did not affect A$\beta$ secretion. Proteomics/cell-based experiments showed that ADAM30-dependent regulation of APP metabolism required both cathepsin D (CTSD) activation and APP sorting to lysosomes. Accordingly, in Alzheimer-like transgenic mice, neuronal ADAM30 over-expression lowered A$\beta$42 secretion in neuron primary cultures, soluble A$\beta$42 and amyloid plaque load levels in the brain and concomitantly enhanced CTSD activity and finally rescued long term potentiation.

in q-bio.NC updates on arXiv.org on June 19, 2019 01:30 AM.

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Bayesian fusion and multimodal DCM for EEG and fMRI. (arXiv:1906.07354v1 [q-bio.QM])

This paper asks whether integrating multimodal EEG and fMRI data offers a better characterisation of functional brain architectures than either modality alone. This evaluation rests upon a dynamic causal model that generates both EEG and fMRI data from the same neuronal dynamics. We introduce the use of Bayesian fusion to provide informative (empirical) neuronal priors - derived from dynamic causal modelling (DCM) of EEG data - for subsequent DCM of fMRI data. To illustrate this procedure, we generated synthetic EEG and fMRI timeseries for a mismatch negativity (or auditory oddball) paradigm, using biologically plausible model parameters (i.e., posterior expectations from a DCM of empirical, open access, EEG data). Using model inversion, we found that Bayesian fusion provided a substantial improvement in marginal likelihood or model evidence, indicating a more efficient estimation of model parameters, in relation to inverting fMRI data alone. We quantified the benefits of multimodal fusion with the information gain pertaining to neuronal and haemodynamic parameters - as measured by the Kullback-Leibler divergence between their prior and posterior densities. Remarkably, this analysis suggested that EEG data can improve estimates of haemodynamic parameters; thereby furnishing proof-of-principle that Bayesian fusion of EEG and fMRI is necessary to resolve conditional dependencies between neuronal and haemodynamic estimators. These results suggest that Bayesian fusion may offer a useful approach that exploits the complementary temporal (EEG) and spatial (fMRI) precision of different data modalities. We envisage the procedure could be applied to any multimodal dataset that can be explained by a DCM with a common neuronal parameterisation.

in q-bio.NC updates on arXiv.org on June 19, 2019 01:30 AM.

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Brain Maturation Study during Adolescence Using Graph Laplacian Learning Based Fourier Transform. (arXiv:1906.07211v1 [q-bio.NC])

Objective: Longitudinal neuroimaging studies have demonstrated that adolescence is the crucial developmental epoch of continued brain growth and change. A large number of researchers dedicate to uncovering the mechanisms about brain maturity during adolescence. Motivated by both achievement in graph signal processing and recent evidence that some brain areas act as hubs connecting functionally specialized systems, we proposed an approach to detect these regions from spectral analysis perspective. In particular, as human brain undergoes substantial development throughout adolescence, we addressed the challenge by evaluating the functional network difference among age groups from functional magnetic resonance imaging (fMRI) observations. Methods: We treated these observations as graph signals defined on the parcellated functional brain regions and applied graph Laplacian learning based Fourier Transform (GLFT) to transform the original graph signals into frequency domain. Eigen-analysis was conducted afterwards to study the behavior of the corresponding brain regions, which enables the characterization of brain maturation. Result: We first evaluated our method on the synthetic data and further applied the method to resting and task state fMRI imaging data from Philadelphia Neurodevelopmental Cohort (PNC) dataset, comprised of normally developing adolescents from 8 to 22. The model provided a highest accuracy of 95.69% in distinguishing different adolescence stages. Conclusion: We detected 13 hubs from resting state fMRI and 16 hubs from task state fMRI that are highly related to brain maturation process. Significance: The proposed GLFT method is powerful in extracting the brain connectivity patterns and identifying hub regions with a high prediction power

in q-bio.NC updates on arXiv.org on June 19, 2019 01:30 AM.

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Classification of Subcortical Vascular Cognitive Impairment Using Single MRI Sequence and Deep Learning Convolutional Neural Networks

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 19, 2019 12:00 AM.

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Impaired Motor Skill Acquisition Using Mirror Visual Feedback Improved by Transcranial Direct Current Stimulation (tDCS) in Patients With Parkinson’s Disease

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 19, 2019 12:00 AM.

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Non-pulsed Sinusoidal Electromagnetic Field Rescues Animals From Severe Ischemic Stroke via NO Activation

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 19, 2019 12:00 AM.

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Measuring Sharp Waves and Oscillatory Population Activity With the Genetically Encoded Calcium Indicator GCaMP6f

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 19, 2019 12:00 AM.

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Convergence of spectrums: neuronal gene network states in autism spectrum disorder

Publication date: December 2019

Source: Current Opinion in Neurobiology, Volume 59

Author(s): Josefa M Sullivan, Silvia De Rubeis, Anne Schaefer

in ScienceDirect Publication: Current Opinion in Neurobiology on June 18, 2019 11:00 PM.

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Transcriptomic correlates of electrophysiological and morphological diversity within and across excitatory and inhibitory neuron classes

by Claire Bomkamp, Shreejoy J. Tripathy, Carolina Bengtsson Gonzales, Jens Hjerling-Leffler, Ann Marie Craig, Paul Pavlidis

in PLOS Computational Biology: New Articles on June 18, 2019 09:00 PM.

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Hierarchical Bayesian inference for concurrent model fitting and comparison for group studies

by Payam Piray, Amir Dezfouli, Tom Heskes, Michael J. Frank, Nathaniel D. Daw

in PLOS Computational Biology: New Articles on June 18, 2019 09:00 PM.

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Correction for Jang et al., Processing bodies control the selective translation for optimal development of Arabidopsis young seedlings [Correction]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Correction for Dutta et al., Regulation of myelin structure and conduction velocity by perinodal astrocytes [Correction]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Correction for Li et al., Activation of RNase L is dependent on OAS3 expression during infection with diverse human viruses [Correction]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Correction for Lorenzo et al., Computer simulations suggest that prostate enlargement due to benign prostatic hyperplasia mechanically impedes prostate cancer growth [Correction]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Elephants have a nose for quantity [Psychological and Cognitive Sciences]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Plant-derived coumarins shape the composition of an Arabidopsis synthetic root microbiome [Plant Biology]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Engineering the phototropin photocycle improves photoreceptor performance and plant biomass production [Plant Biology]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Arabidopsis ABCG28 is required for the apical accumulation of reactive oxygen species in growing pollen tubes [Plant Biology]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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The Cdk1/Cdk2 homolog CDKA;1 controls the recombination landscape in Arabidopsis [Plant Biology]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Specific factors in blood from young but not old mice directly promote synapse formation and NMDA-receptor recruitment [Neuroscience]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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NRF2/ARE pathway negatively regulates BACE1 expression and ameliorates cognitive deficits in mouse Alzheimer’s models [Neuroscience]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Routing information flow by separate neural synchrony frequencies allows for “functionally labeled lines” in higher primate cortex [Neuroscience]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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UBE3A-mediated PTPA ubiquitination and degradation regulate PP2A activity and dendritic spine morphology [Neuroscience]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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ANO1/TMEM16A regulates process maturation in radial glial cells in the developing brain [Neuroscience]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Stress transforms lateral habenula reward responses into punishment signals [Neuroscience]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Primary structural differences at residue 226 of deer and elk PrP dictate selection of distinct CWD prion strains in gene-targeted mice [Microbiology]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Ammonia generation by tryptophan synthase drives a key genetic difference between genital and ocular Chlamydia trachomatis isolates [Microbiology]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Salmonella biofilms program innate immunity for persistence in Caenorhabditis elegans [Microbiology]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Hypoxia-induced switch in SNAT2/SLC38A2 regulation generates endocrine resistance in breast cancer [Medical Sciences]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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JAK/STAT inhibition in macrophages promotes therapeutic resistance by inducing expression of protumorigenic factors [Medical Sciences]

in Proceedings of the National Academy of Sciences Recent Issues on June 18, 2019 04:48 PM.

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Transcranial Direct Current Stimulation Effects on Memory Consolidation: Timing Matters

Transcranial direct current stimulation (tDCS) is a promising tool for modulation of learning and memory, allowing to transiently change cortical excitability of specific brain regions with physiological and behavioral outcomes. A detailed exploration of factors that can moderate tDCS effects on episodic long-term memory (LTM) is of high interest due to the clinical potential for patients with traumatic or pathological memory deficits and with cognitive impairments. This commentary discusses findings by Marián et al. (2018) recently published in Cortex within a broad context of brain stimulation in memory research.

in eNeuro current issue on June 18, 2019 04:32 PM.

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Slow NMDA-Mediated Excitation Accelerates Offset-Response Latencies Generated via a Post-Inhibitory Rebound Mechanism

In neural circuits, action potentials (spikes) are conventionally caused by excitatory inputs whereas inhibitory inputs reduce or modulate neuronal excitability. We previously showed that neurons in the superior paraolivary nucleus (SPN) require solely synaptic inhibition to generate their hallmark offset response, a burst of spikes at the end of a sound stimulus, via a post-inhibitory rebound mechanism. In addition SPN neurons receive excitatory inputs, but their functional significance is not yet known. Here we used mice of both sexes to demonstrate that in SPN neurons, the classical roles for excitation and inhibition are switched, with inhibitory inputs driving spike firing and excitatory inputs modulating this response. Hodgkin–Huxley modeling suggests that a slow, NMDA receptor (NMDAR)-mediated excitation would accelerate the offset response. We find corroborating evidence from in vitro and in vivo recordings that lack of excitation prolonged offset-response latencies and rendered them more variable to changing sound intensity levels. Our results reveal an unsuspected function for slow excitation in improving the timing of post-inhibitory rebound firing even when the firing itself does not depend on excitation. This shows the auditory system employs highly specialized mechanisms to encode timing-sensitive features of sound offsets which are crucial for sound-duration encoding and have profound biological importance for encoding the temporal structure of speech.

in eNeuro current issue on June 18, 2019 04:30 PM.

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Molecular, Morphological, and Functional Characterization of Corticotropin-Releasing Factor Receptor 1-Expressing Neurons in the Central Nucleus of the Amygdala

The central nucleus of the amygdala (CeA) is a brain region implicated in anxiety, stress-related disorders and the reinforcing effects of drugs of abuse. Corticotropin-releasing factor (CRF, Crh) acting at cognate type 1 receptors (CRF₁, Crhr1) modulates inhibitory and excitatory synaptic transmission in the CeA. Here, we used CRF₁:GFP reporter mice to characterize the morphological, neurochemical and electrophysiological properties of CRF₁-expressing (CRF₁+) and CRF₁-non-expressing (CRF₁–) neurons in the CeA. We assessed these two neuronal populations for distinctions in the expression of GABAergic subpopulation markers and neuropeptides, dendritic spine density and morphology, and excitatory transmission. We observed that CeA CRF₁+ neurons are GABAergic but do not segregate with calbindin (CB), calretinin (CR), parvalbumin (PV), or protein kinase C- (PKC). Among the neuropeptides analyzed, Penk and Sst had the highest percentage of co-expression with Crhr1 in both the medial and lateral CeA subdivisions. Additionally, CeA CRF₁+ neurons had a lower density of dendritic spines, which was offset by a higher proportion of mature spines compared to neighboring CRF₁– neurons. Accordingly, there was no difference in basal spontaneous glutamatergic transmission between the two populations. Application of CRF increased overall vesicular glutamate release onto both CRF₁+ and CRF₁– neurons and does not affect amplitude or kinetics of EPSCs in either population. These novel data highlight important differences in the neurochemical make-up and morphology of CRF₁+ compared to CRF₁– neurons, which may have important implications for the transduction of CRF signaling in the CeA.

in eNeuro current issue on June 18, 2019 04:30 PM.

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Rapid online learning and robust recall in a neuromorphic olfactory circuit. (arXiv:1906.07067v1 [cs.NE])

The mammalian olfactory system learns new odors rapidly, exhibits negligible interference among odor memories, and identifies known odors under challenging conditions. The mechanisms by which it does so are unknown. We here present a general theory for odor learning and identification under noise in the olfactory system, and demonstrate its efficacy using a neuromorphic model of the olfactory bulb. As with biological olfaction, the spike timing-based algorithm utilizes distributed, event-driven computations and rapid online learning. Localized spike timing-dependent plasticity rules are employed iteratively over sequential gamma-frequency packets to construct odor representations from the activity of chemosensor arrays mounted in a wind tunnel. Learned odors then are reliably identified despite strong destructive interference. Noise resistance is enhanced by neuromodulation and contextual priming. Lifelong learning capabilities are enabled by adult neurogenesis. The algorithm is applicable to any signal identification problem in which high-dimensional signals are embedded in unknown backgrounds.

in q-bio.NC updates on arXiv.org on June 18, 2019 01:30 AM.

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Brain Controllability: not a slam dunk yet. (arXiv:1906.06778v1 [q-bio.QM])

In our recent article (Tu et al., Warnings and caveats in brain controllability, arXiv:1705.08261) we provided quantitative evidence to show that there are warnings and caveats in the way Gu and collaborators (Gu et al. Controllability of structural brain networks. Nature communications 6 (2015): 8414) define brain controllability. The comment by Pasqualetti et al. (Pasqualetti et al. RE: Warnings and Caveats in Brain Controllability. NeuroImage 297 (2019), 586-588) confirms the need to go beyond the methodology and approach presented in Gu et al. original work. In fact, they recognize that the source of confusion is due to the fact that assessing controllability via numerical analysis typically leads to ill-conditioned problems, and thus often generates results that are difficult to interpret. This is indeed the first warning we discussed: our work was not meant to prove that brain networks are not controllable from one node, rather we wished to highlight that the one node controllability framework and all consequent results were not properly justified based on the methodology presented in Gu et al. We used in our work the same method of Gu et al. not because we believe it is the best methodology, but because we extensively investigated it with the aim of replicating, testing and extending their results. And the warning and caveats we have proposed are the results of this investigation.

in q-bio.NC updates on arXiv.org on June 18, 2019 01:30 AM.

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Agito ergo sum: correlates of spatiotemporal motion characteristics during fMRI. (arXiv:1906.06445v1 [q-bio.NC])

The impact of in-scanner motion on functional magnetic resonance imaging (fMRI) data has a notorious reputation in the neuroimaging community. State-ofthe-art guidelines advise to scrub out excessively corrupted frames as assessed by a composite framewise displacement (FD) score, to regress out models of nuisance variables, and to include average FD as a covariate in group-level analyses.

Here, we studied individual motion time courses at time points typically retained in fMRI analyses. We observed that even in this set of putatively clean time points, motion exhibited a very clear spatiotemporal structure, so that we could distinguish subjects into four groups of movers with varying characteristics

Then, we showed that this spatiotemporal motion cartography tightly relates to a broad array of anthropometric, behavioral and clinical factors. Convergent results were obtained from two different analytical perspectives: univariate assessment of behavioral differences across mover subgroups unraveled defining markers, while subsequent multivariate analysis broadened the range of involved factors and clarified that multiple motion/behavior modes of covariance overlap in the data.

Our results demonstrate that even the smaller episodes of motion typically retained in fMRI analyses carry structured, behaviorally relevant information. They call for further examinations of possible biases in current regression-based motion correction strategies.

in q-bio.NC updates on arXiv.org on June 18, 2019 01:30 AM.

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Blocking facial mimicry selectively alters early stages of facial expression processing. (arXiv:1906.06424v1 [q-bio.NC])

Simulation models of facial expressions suggest that posterior visual areas and brain areas underpinning sensorimotor simulations might interact to improve facial expression processing. According to these models, facial mimicry may contribute to the visual perceptual processing of facial expressions by influencing early stages of face processing, thus playing a crucial role in understanding the observed emotion. The aim of the present study was to assess whether and how early sensorimotor simulation influences face structural encoding/processing. A secondary aim was to investigate whether there is a relationship between alexithymic traits and sensorimotor simulation as a mechanism for fine facial expression discrimination. In order to examine the time-course of face processing, we monitored P1 and N170 components of the event-related potentials (ERP) in participants performing a fine discrimination task of facial expressions. An animal discrimination task was implemented as a control condition. In half of the experiment, participants could freely use their facial mimicry whereas, in the other half, they had their facial mimicry blocked by a gel. Our results revealed that the P1 ERP component was not modulated by the mimicry manipulation while the N170 amplitude was larger in the blocked mimicry condition when compared to the free mimicry condition selectively for the face stimuli. Interestingly, this modulation interacted with the alexithymic traits, with a reduction of the N170 amplitude modulation as a function of the facial mimicry manipulation for participants with the highest levels of alexithymic traits. These results demonstrate that sensorimotor simulation influences visual processing of facial expressions at early stages and that participants with higher alexithymic traits tend to underutilize the sensorimotor simulation system.

in q-bio.NC updates on arXiv.org on June 18, 2019 01:30 AM.

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Releasing the brake

Nature Reviews Neuroscience, Published online: 18 June 2019; doi:10.1038/s41583-019-0199-0

in Nature Reviews Neuroscience - Issue - nature.com science feeds on June 18, 2019 12:00 AM.

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Shank3 Mice Carrying the Human Q321R Mutation Display Enhanced Self-Grooming, Abnormal Electroencephalogram Patterns, and Suppressed Neuronal Excitability and Seizure Susceptibility

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 18, 2019 12:00 AM.

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A Critical Period for the Development of Schizophrenia-Like Pathology by Aberrant Postnatal Neurogenesis

in Frontiers in Neuroscience | Neurogenesis section | New and Recent Articles on June 18, 2019 12:00 AM.

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Altered Insulin Signaling in Alzheimer’s Disease Brain – Special Emphasis on PI3K-Akt Pathway

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 18, 2019 12:00 AM.

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Objective and Automated Detection of Diffuse White Matter Abnormality in Preterm Infants Using Deep Convolutional Neural Networks

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 18, 2019 12:00 AM.

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New Neurons in the Post-ischemic and Injured Brain: Migrating or Resident?

in Frontiers in Neuroscience | Neurogenesis section | New and Recent Articles on June 18, 2019 12:00 AM.

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Prion-Like Mechanisms in Parkinson’s Disease

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 18, 2019 12:00 AM.

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Interpreting Prefrontal Recruitment During Walking After Stroke: Influence of Individual Differences in Mobility and Cognitive Function

in Frontiers in Human Neuroscience | New and Recent Articles on June 18, 2019 12:00 AM.

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Abnormal Interactions of the Salience Network, Central Executive Network, and Default-Mode Network in Patients With Different Cognitive Impairment Loads Caused by Leukoaraiosis

in Frontiers in Neural Circuits | New and Recent Articles on June 18, 2019 12:00 AM.

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Secretion of Mast Cell Inflammatory Mediators Is Enhanced by CADM1-Dependent Adhesion to Sensory Neurons

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 18, 2019 12:00 AM.

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Distinct Brain Regions in Physiological and Pathological Brain Aging

in Frontiers in Aging Neuroscience | New and Recent Articles on June 18, 2019 12:00 AM.

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Effects of tDCS of Dorsolateral Prefrontal Cortex on Dual-Task Performance Involving Manual Dexterity and Cognitive Task in Healthy Older Adults

in Frontiers in Aging Neuroscience | New and Recent Articles on June 18, 2019 12:00 AM.

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The Gut-Brain Axis in Neurodegenerative Diseases and Relevance of the Canine Model: A Review

in Frontiers in Aging Neuroscience | New and Recent Articles on June 18, 2019 12:00 AM.

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Seizing an opportunity

in eLife: latest articles on June 18, 2019 12:00 AM.

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A lesson in homology

in eLife: latest articles on June 18, 2019 12:00 AM.

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Structure of the Helicobacter pylori Cag Type IV secretion system

in eLife: latest articles on June 18, 2019 12:00 AM.

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Variable opportunities for outcrossing result in hotspots of novel genetic variation in a pathogen metapopulation

in eLife: latest articles on June 18, 2019 12:00 AM.

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Cretaceous dinosaur bone contains recent organic material and provides an environment conducive to microbial communities

in eLife: latest articles on June 18, 2019 12:00 AM.

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Family history of Alzheimer's disease alters cognition and is modified by medical and genetic factors

in eLife: latest articles on June 18, 2019 12:00 AM.

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Cryo-EM structures of remodeler-nucleosome intermediates suggest allosteric control through the nucleosome

in eLife: latest articles on June 18, 2019 12:00 AM.

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A FRET sensor of C-terminal movement reveals VRAC activation by plasma membrane DAG signaling rather than ionic strength

in eLife: latest articles on June 18, 2019 12:00 AM.

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Evolution of limb development in cephalopod mollusks

in eLife: latest articles on June 18, 2019 12:00 AM.

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Neuromodulation Leads to a Burst-Tonic Switch in a Subset of VIP Neurons in Mouse Primary Somatosensory (Barrel) Cortex

in Cerebral Cortex Open Access on June 18, 2019 12:00 AM.

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Unusual Physiological Properties of Smooth Monostratified Ganglion Cell Types in Primate Retina

in Neuron on June 18, 2019 12:00 AM.

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Rapid Reconfiguration of the Functional Connectome after Chemogenetic Locus Coeruleus Activation

in Neuron on June 18, 2019 12:00 AM.

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Neural, functional, and aesthetic impacts of spatially heterogeneous flicker: A potential role of natural flicker

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Exploratory Data Analysis in The Vallecas Project: A six years longitudinal study in healthy brain aging

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Physical activity, aerobic fitness and brain white matter: their role for executive functions in adolescence

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Serotonin Neurons in the Dorsal and Medial Raphe Nuclei: from Single-Cell Transcriptomes to Whole-Brain Projections

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Nucleus Basalis Stimulation Stabilizes Attractor Networks and Enhances Task Representation in Prefrontal Cortex

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Altered dorsal CA1 neuronal population coding in the APP/PS1 mouse model of Alzheimer\'s disease

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Chronic Stability of Single-Channel Neurophysiological Correlates of Gross and Fine Reaching Movements in the Rat

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Maximizing the coding capacity of neuronal networks

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Calretinin positive neurons form an excitatory amplifier network in the spinal cord dorsal horn

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Highly Accelerated Vessel-Selective Arterial Spin Labelling Angiography using Sparsity and Smoothness Constraints

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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PET and CSF amyloid-β status are differently predicted by patient features: Information from discordant cases

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Cervical spinal cord atrophy and Alzheimer\'s disease.

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Functions of ventral visual cortex after bilateral hippocampal loss

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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High Throughput Evolution of Near Infrared Serotonin Nanosensors

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Reconstruction of in-vivo subthreshold activity of single neurons from large-scale spiking recordings

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Subcortical brain volume, regional cortical thickness and cortical surface area across attention-deficit/hyperactivity disorder (ADHD), autism spectrum disorder (ASD), and obsessive-compulsive disorder (OCD): findings from the ENIGMA-ADHD, -ASD, and -OCD working groups

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Towards an Objective Evaluation of EEG/MEG Source Estimation Methods: The Linear Tool Kit

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Paying Attention to Speech: The Role of Cognitive Capacity and Acquired Experience

in bioRxiv Subject Collection: Neuroscience on June 18, 2019 12:00 AM.

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Correction: Path Similarity Analysis: A Method for Quantifying Macromolecular Pathways

by Sean L. Seyler, Avishek Kumar, M. F. Thorpe, Oliver Beckstein

in PLOS Computational Biology: New Articles on June 17, 2019 09:00 PM.

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Correction: Recentrifuge: Robust comparative analysis and contamination removal for metagenomics

by Jose Manuel Martí

in PLOS Computational Biology: New Articles on June 17, 2019 09:00 PM.

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A multi-scale model of gas transport in the lung to study heterogeneous lung ventilation during the multiple-breath washout test

by David Hasler, Pinelopi Anagnostopoulou, Sylvia Nyilas, Philipp Latzin, Johannes Schittny, Dominik Obrist

in PLOS Computational Biology: New Articles on June 17, 2019 09:00 PM.

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Rational discovery of dual-indication multi-target PDE/Kinase inhibitor for precision anti-cancer therapy using structural systems pharmacology

by Hansaim Lim, Di He, Yue Qiu, Patrycja Krawczuk, Xiaoru Sun, Lei Xie

in PLOS Computational Biology: New Articles on June 17, 2019 09:00 PM.

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How Do You Treat Traumatic Brain Injury? One Symptom at a Time

in Wiley: Annals of Neurology: Table of Contents on June 17, 2019 06:49 PM.

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Deoxynucleoside Therapy for Thymidine Kinase 2–Deficient Myopathy

Objective

Thymidine kinase 2, encoded by the nuclear gene TK2, is required for mitochondrial DNA maintenance. Autosomal recessive TK2 mutations cause depletion and multiple deletions of mtDNA that manifest predominantly as a myopathy usually beginning in childhood and progressing relentlessly. We investigated the safety and efficacy of deoxynucleoside monophosphate and deoxynucleoside therapies.

Methods

We administered deoxynucleoside monophosphates and deoxynucleoside to 16 TK2‐deficient patients under a compassionate use program.

Results

In 5 patients with early onset and severe disease, survival and motor functions were better than historically untreated patients. In 11 childhood and adult onset patients, clinical measures stabilized or improved. Three of 8 patients who were nonambulatory at baseline gained the ability to walk on therapy; 4 of 5 patients who required enteric nutrition were able to discontinue feeding tube use; and 1 of 9 patients who required mechanical ventilation became able to breathe independently. In motor functional scales, improvements were observed in the 6‐minute walk test performance in 7 of 8 subjects, Egen Klassifikation in 2 of 3, and North Star Ambulatory Assessment in all 5 tested. Baseline elevated serum growth differentiation factor 15 levels decreased with treatment in all 7 patients tested. A side effect observed in 8 of the 16 patients was dose‐dependent diarrhea, which did not require withdrawal of treatment. Among 12 other TK2 patients treated with deoxynucleoside, 2 adults developed elevated liver enzymes that normalized following discontinuation of therapy.

Interpretation

This open‐label study indicates favorable side effect profiles and clinical efficacy of deoxynucleoside monophosphate and deoxynucleoside therapies for TK2 deficiency. ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 17, 2019 06:03 PM.

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Intellectual and Developmental Disabilities Research Centers: 50 Years of Scientific Accomplishments

Abstract

Progress in addressing the origins of intellectual and developmental disabilities accelerated with the establishment 50 years ago of the Eunice Kennedy Shriver National Institute of Child Health and Human Development of the National Institutes of Health and associated Intellectual and Developmental Disabilities Research Centers. Investigators at these Centers have made seminal contributions to understand human brain and behavioral development, and to define mechanisms and treatments of disorders of the developing brain.

This article is protected by copyright. All rights reserved.

in Wiley: Annals of Neurology: Table of Contents on June 17, 2019 05:07 PM.

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Cyfip1 haploinsufficiency does not alter GABAA receptor {delta}-subunit expression and tonic inhibition in dentate gyrus PV+ interneurons and granule cells

Copy number variation at chromosomal region 15q11.2 is linked to increased risk of neurodevelopmental disorders including autism and schizophrenia. A significant gene at this locus is cytoplasmic fragile X mental retardation protein (FMRP) interacting protein 1 (CYFIP1). CYFIP1 protein interacts with FMRP, whose monogenic absence causes Fragile X syndrome. FMRP knock-out has been shown to reduce tonic GABAergic inhibition by interacting with the -subunit of the GABA_A receptor. Using in situ hybridization, qPCR, western blot techniques and patch clamp electrophysiology in brain slices from a Cyfip1 haploinsufficient mouse, we examined -subunit mediated tonic inhibition in the dentate gyrus. In wild-type mice, dentate gyrus granule cells (DGGC) responded to the -subunit selective agonist THIP with significantly increased tonic currents. In heterozygous mice, no significant difference was observed in THIP evoked currents in DGGC. Phasic GABAergic inhibition in DGGC was also unaltered with no difference in properties of spontaneous inhibitory post synaptic currents (IPSCs). Additionally, we demonstrate that dentate gyrus granule cell layer PV⁺-interneurons (PV⁺-IN) have functional -subunit mediated tonic GABAergic currents which, unlike DGGC, are also modulated by the α₁ selective drug zolpidem. Similar to DGGC, both IPSCs and THIP-evoked currents in PV⁺-IN were not different between Cyfip1 heterozygous and wild-type mice. Supporting our electrophysiological data, we found no significant change in hippocampal -subunit mRNA expression or protein level and no change in α₁/α₄ subunit mRNA expression. Thus, Cyfip1 haploinsufficiency, mimicking human 15q11.2 microdeletion syndrome, does not alter hippocampal phasic or tonic GABAergic inhibition, substantially differing from the FMRP knock-out mouse model.

Significance StatementCYFIP1 is a candidate risk gene for neurodevelopmental and neuropsychiatric disorders. CYFIP1 protein interacts with FMRP whose loss downregulates tonic GABAergic inhibition via interaction with the -subunit of the GABA_A receptor. Here, however, we report that reduced Cyfip1 dosage in mice does not alter tonic GABAergic inhibition in granule cells and PV⁺-interneurons of the dentate gyrus, a region rich in -subunit expression. Despite these negative findings, our data does demonstrate that PV⁺-interneurons of the DG granule cell layer are functionally regulated by tonic GABAergic inhibition, and in contrast to granule cells, this involves receptors incorporating both and α₁-subunits. Thus, granule cell layer excitatory neurons and PV⁺-interneurons may be differentially modulated by subunit selective GABA receptor targeting drugs.

in RSS PAP on June 17, 2019 04:30 PM.

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Temporal dynamics of inhalation-linked activity across defined subpopulations of mouse olfactory bulb neurons imaged in vivo

In mammalian olfaction, inhalation drives the temporal patterning of neural activity that underlies early olfactory processing. It remains poorly understood how the neural circuits that process incoming olfactory information are engaged in the context of inhalation-linked dynamics. Here, we used artificial inhalation and two-photon calcium imaging to compare the dynamics of activity evoked by odorant inhalation across major cell types of the mouse olfactory bulb (OB). We expressed GCaMP6f or jRGECO1a in mitral and tufted cell subpopulations, olfactory sensory neurons, and two major juxtaglomerular interneuron classes, and imaged responses to a single inhalation of odorant. Activity in all cell types was strongly linked to inhalation, and all cell types showed some variance in the latency, rise-times, and durations of their inhalation-linked response. Juxtaglomerular interneuron dynamics closely matched that of sensory inputs, while mitral and tufted cells showed the highest diversity in responses, with a range of latencies and durations that could not be accounted for by heterogeneity in sensory input dynamics. Diversity was apparent even among 'sister' tufted cells innervating the same glomerulus. Surprisingly, inhalation-linked responses of mitral and tufted cells were highly overlapping and could not be distinguished on the basis of their inhalation-linked dynamics, with the exception of a subpopulation of superficial tufted cells expressing cholecystokinin. Our results are consistent with a model in which diversity in inhalation-linked patterning of OB output arises first at the level of sensory input and is enhanced by feedforward inhibition from juxtaglomerular interneurons which differentially impact different subpopulations of OB output neurons.

SIGNIFICANCE STATEMENT Inhalation drives the temporal patterning of neural activity that underlies olfactory processing and rapid odor perception, yet the dynamics of the neural circuit elements mediating this processing are poorly understood. By comparing inhalation-linked dynamics of major olfactory bulb subpopulations, we find that diversity in the timing of neural activation arises at the level of sensory input, which is then mirrored by inhibitory interneurons in the glomerular layer. Temporal diversity is higher among olfactory bulb output neurons, with different subpopulations showing distinct but nonetheless highly overlapping ranges of inhalation-linked dynamics. These results implicate feedforward inhibition by glomerular-layer interneurons in diversifying temporal responses among output neurons, which may be important for generating and shaping timing-based odor representations during natural odor sampling.

in RSS PAP on June 17, 2019 04:30 PM.

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The scientific case for brain simulations. (arXiv:1906.06189v1 [q-bio.NC])

A key element of the European Union's Human Brain Project (HBP) and other large-scale brain research projects is simulation of large-scale model networks of neurons. Here we argue why such simulations will likely be indispensable for bridging the scales between the neuron and system levels in the brain, and a set of brain simulators based on neuron models at different levels of biological detail should thus be developed. To allow for systematic refinement of candidate network models by comparison with experiments, the simulations should be multimodal in the sense that they should not only predict action potentials, but also electric, magnetic, and optical signals measured at the population and system levels.

in q-bio.NC updates on arXiv.org on June 17, 2019 01:30 AM.

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Imperfect fifths pack into musical scales. (arXiv:1906.06171v1 [cs.SD])

Musical scales are used in cultures throughout the world, but the question as to how they evolved remains open. Some suggest that scales based on the harmonic series are inherently pleasant, while others propose that scales are chosen that are easy to sing, hear and reproduce accurately. However, testing these theories has been hindered by the sparseness of empirical evidence. Here, to enable such examination, we assimilate data from diverse ethnomusicological sources into a cross-cultural database of scales. We generate populations of scales based on proposed and alternative theories and assess their similarity to empirical distributions from the database. Most scales can be explained as tending to include intervals roughly corresponding to perfect fifths ("imperfect fifths"), and packing arguments explain the salient features of the distributions. Scales are also preferred if their intervals are compressible, which could facilitate efficient communication and memory of melodies. While no single theory can explain all scales, which appear to evolve according to different selection pressures, the simplest harmonicity-based, imperfect-fifths packing model best fits the empirical data.

in q-bio.NC updates on arXiv.org on June 17, 2019 01:30 AM.

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Periodic Codes and Sound Localization. (arXiv:1906.06006v1 [q-bio.NC])

Inspired by the sound localization system of the barn owl, we define a new class of neural codes, called periodic codes, and study their basic properties. Periodic codes are binary codes with a special patterned form that reflects the periodicity of the stimulus. Because these codes can be used by the owl to localize sounds within a convex set of angles, we investigate whether they are examples of convex codes, which have previously been studied for hippocampal place cells. We find that periodic codes are typically not convex, but can be completed to convex codes in the presence of noise. We introduce the convex closure and Hamming distance completion as ways of adding codewords to make a code convex, and describe the convex closure of a periodic code. We also find that the probability of the convex closure arising stochastically is greater for sparser codes. Finally, we provide an algebraic method using the neural ideal to detect if a code is periodic. We find that properties of periodic codes help to explain several aspects of the behavior observed in the sound localization system of the barn owl, including common errors in localizing pure tones.

in q-bio.NC updates on arXiv.org on June 17, 2019 01:30 AM.

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Hot topic in optogenetics: new implications of in vivo tissue heating

Nature Neuroscience, Published online: 17 June 2019; doi:10.1038/s41593-019-0426-z

in Nature Neuroscience - Issue - nature.com science feeds on June 17, 2019 12:00 AM.

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Thermal constraints on in vivo optogenetic manipulations

Nature Neuroscience, Published online: 17 June 2019; doi:10.1038/s41593-019-0422-3

in Nature Neuroscience - Issue - nature.com science feeds on June 17, 2019 12:00 AM.

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Morphine withdrawal recruits lateral habenula cytokine signaling to reduce synaptic excitation and sociability

Nature Neuroscience, Published online: 17 June 2019; doi:10.1038/s41593-019-0421-4

in Nature Neuroscience - Issue - nature.com science feeds on June 17, 2019 12:00 AM.

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Sensory lesioning induces microglial synapse elimination via ADAM10 and fractalkine signaling

Nature Neuroscience, Published online: 17 June 2019; doi:10.1038/s41593-019-0419-y

in Nature Neuroscience - Issue - nature.com science feeds on June 17, 2019 12:00 AM.

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Classification of electrophysiological and morphological neuron types in the mouse visual cortex

Nature Neuroscience, Published online: 17 June 2019; doi:10.1038/s41593-019-0417-0

in Nature Neuroscience - Issue - nature.com science feeds on June 17, 2019 12:00 AM.

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Genome-wide association study implicates CHRNA2 in cannabis use disorder

Nature Neuroscience, Published online: 17 June 2019; doi:10.1038/s41593-019-0416-1

in Nature Neuroscience - Issue - nature.com science feeds on June 17, 2019 12:00 AM.

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Acetic acid activates distinct taste pathways in Drosophila to elicit opposing, state-dependent feeding responses

in eLife: latest articles on June 17, 2019 12:00 AM.

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Pregnancy-associated plasma protein-aa supports hair cell survival by regulating mitochondrial function

in eLife: latest articles on June 17, 2019 12:00 AM.

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Cystic fibrosis drug ivacaftor stimulates CFTR channels at picomolar concentrations

in eLife: latest articles on June 17, 2019 12:00 AM.

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Absolute quantification of cohesin, CTCF and their regulators in human cells

in eLife: latest articles on June 17, 2019 12:00 AM.

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Cas9⁺ conditionally-immortalized macrophages as a tool for bacterial pathogenesis and beyond

in eLife: latest articles on June 17, 2019 12:00 AM.

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Rapid and iterative genome editing in the malaria parasite Plasmodium knowlesi provides new tools for P. vivax research

in eLife: latest articles on June 17, 2019 12:00 AM.

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Conformational switches control early maturation of the eukaryotic small ribosomal subunit

in eLife: latest articles on June 17, 2019 12:00 AM.

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Liquid-crystal organization of liver tissue

in eLife: latest articles on June 17, 2019 12:00 AM.

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Anatomical and physiological foundations of cerebello-hippocampal interaction

in eLife: latest articles on June 17, 2019 12:00 AM.

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Determining cellular CTCF and cohesin abundances to constrain 3D genome models

in eLife: latest articles on June 17, 2019 12:00 AM.

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Extracellular Pax6 Regulates Tangential Cajal–Retzius Cell Migration in the Developing Mouse Neocortex

in Cerebral Cortex Advance Access on June 17, 2019 12:00 AM.

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Brain State-dependent Gain Modulation of Corticospinal Output in the Active Motor System

in Cerebral Cortex Advance Access on June 17, 2019 12:00 AM.

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High-Frequency Activation of Nucleus Accumbens D1-MSNs Drives Excitatory Potentiation on D2-MSNs

in Neuron on June 17, 2019 12:00 AM.

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Neuronally Enriched RUFY3 Is Required for Caspase-Mediated Axon Degeneration

in Neuron on June 17, 2019 12:00 AM.

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The involvement of spinal annexin A10/NF-κB/MMP-9 pathway in the development of neuropathic pain in rats

in Most Recent Articles: BMC Neuroscience on June 17, 2019 12:00 AM.

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Gastrodin protects dopaminergic neurons via insulin-like pathway in a Parkinson’s disease model

in Most Recent Articles: BMC Neuroscience on June 17, 2019 12:00 AM.

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Live calcium imaging of Aedes aegypti neuronal tissues reveals differential importance of chemosensory systems for life-history-specific foraging strategies

in Most Recent Articles: BMC Neuroscience on June 17, 2019 12:00 AM.

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Evaluation of IL-1β levels in epilepsy and traumatic brain injury in dogs

in Most Recent Articles: BMC Neuroscience on June 17, 2019 12:00 AM.

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Abnormal resting-state cerebral-limbic functional connectivity in bipolar depression and unipolar depression

in Most Recent Articles: BMC Neuroscience on June 17, 2019 12:00 AM.

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Regulation of perineuronal nets in the adult cortex by the electrical activity of parvalbumin interneurons

in bioRxiv Subject Collection: Neuroscience on June 17, 2019 12:00 AM.

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Neuron-Glial Antigen 2 (NG2)-based Glial Induction ofHuman BMSCs: A fast & safe glial progenitor cell-based therapy for congenital myelin disorders of the central nervous system

in bioRxiv Subject Collection: Neuroscience on June 17, 2019 12:00 AM.

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A Review of Recurrent Neural Networks: LSTM Cells and Network Architectures

in MIT Press: Neural Computation: Table of Contents on June 15, 2019 04:22 AM.

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A Reservoir Computing Model of Reward-Modulated Motor Learning and Automaticity

in MIT Press: Neural Computation: Table of Contents on June 15, 2019 04:21 AM.

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A Computational Perspective of the Role of the Thalamus in Cognition

in MIT Press: Neural Computation: Table of Contents on June 15, 2019 04:21 AM.

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Effect of Depth and Width on Local Minima in Deep Learning

in MIT Press: Neural Computation: Table of Contents on June 15, 2019 04:21 AM.

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Characterizing Brain Connectivity From Human Electrocorticography Recordings With Unobserved Inputs During Epileptic Seizures

in MIT Press: Neural Computation: Table of Contents on June 15, 2019 04:21 AM.

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Multi-Input, Multi-Output Neuronal Mode Network Approach to Modeling the Encoding Dynamics and Functional Connectivity of Neural Systems

in MIT Press: Neural Computation: Table of Contents on June 15, 2019 04:21 AM.

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Effective Dimensionality Reduction for Visualizing Neural Dynamics by Laplacian Eigenmaps

in MIT Press: Neural Computation: Table of Contents on June 15, 2019 04:21 AM.

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Matrix Product State–Based Quantum Classifier

in MIT Press: Neural Computation: Table of Contents on June 15, 2019 04:21 AM.

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A Case of Near-Optimal Sensory Integration Based on Kohonen Self-Organizing Maps

in MIT Press: Neural Computation: Table of Contents on June 15, 2019 04:20 AM.

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Neuronal Regulation of Immunity in the Skin and Lungs

in Trends in Neurosciences on June 15, 2019 12:00 AM.

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Correction: Geospatial characteristics of measles transmission in China during 2005−2014

by Wan Yang, Liang Wen, Shen-Long Li, Kai Chen, Wen-Yi Zhang, Jeffrey Shaman

in PLOS Computational Biology: New Articles on June 14, 2019 09:00 PM.

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Correction: Most Undirected Random Graphs Are Amplifiers of Selection for Birth-Death Dynamics, but Suppressors of Selection for Death-Birth Dynamics

by The PLOS Computational Biology Staff

in PLOS Computational Biology: New Articles on June 14, 2019 09:00 PM.

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Correction: Ten Simple Rules for Taking Advantage of Git and GitHub

by The PLOS Computational Biology Staff

in PLOS Computational Biology: New Articles on June 14, 2019 09:00 PM.

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Correction: Deciphering Signaling Pathway Networks to Understand the Molecular Mechanisms of Metformin Action

by The PLOS Computational Biology Staff

in PLOS Computational Biology: New Articles on June 14, 2019 09:00 PM.

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Correction: The Equivalence of Information-Theoretic and Likelihood-Based Methods for Neural Dimensionality Reduction

by The PLOS Computational Biology Staff

in PLOS Computational Biology: New Articles on June 14, 2019 09:00 PM.

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Correction: Effects of Darwinian Selection and Mutability on Rate of Broadly Neutralizing Antibody Evolution during HIV-1 Infection

by The PLOS Computational Biology Staff

in PLOS Computational Biology: New Articles on June 14, 2019 09:00 PM.

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Correction: Reconstructible Phylogenetic Networks: Do Not Distinguish the Indistinguishable

by The PLOS Computational Biology Staff

in PLOS Computational Biology: New Articles on June 14, 2019 09:00 PM.

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DeepConv-DTI: Prediction of drug-target interactions via deep learning with convolution on protein sequences

by Ingoo Lee, Jongsoo Keum, Hojung Nam

in PLOS Computational Biology: New Articles on June 14, 2019 09:00 PM.

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Pathogenicity and functional impact of non-frameshifting insertion/deletion variation in the human genome

by Kymberleigh A. Pagel, Danny Antaki, AoJie Lian, Matthew Mort, David N. Cooper, Jonathan Sebat, Lilia M. Iakoucheva, Sean D. Mooney, Predrag Radivojac

in PLOS Computational Biology: New Articles on June 14, 2019 09:00 PM.

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Different microvascular alterations underlie microbleeds and microinfarcts

Objective

Cerebral amyloid angiopathy (CAA) is characterized by the accumulation of amyloid β (Aβ) in the walls of cortical vessels and the accrual of microbleeds and microinfarcts over time. The relationship between CAA severity and microbleeds and microinfarcts as well as the sequence of events that lead to lesion formation remain poorly understood.

Methods

We scanned intact formalin‐fixed hemispheres of 12 CAA cases with magnetic resonance imaging (MRI), followed by histopathological examination in predefined areas and serial sectioning in targeted areas with multiple lesions.

Results

In total, 1,168 cortical microbleeds and 472 cortical microinfarcts were observed on ex vivo MRI. Increasing CAA severity at the whole‐brain or regional level was not associated with the number of microbleeds or microinfarcts. However, locally, the density of Aβ‐positive cortical vessels was lower surrounding a microbleed compared to a simulated control lesion, and higher surrounding microinfarcts. Serial sectioning revealed that for (n = 28) microbleeds, both Aβ (4%) and smooth muscle cells (4%) were almost never present in the vessel wall at the site of bleeding, but Aβ was frequently observed upstream or downstream (71%), as was extensive fibrin(ogen) buildup (87%). In contrast, for (n = 22) microinfarcts, vascular Aβ was almost always observed at the core of the lesion (91%, p < 0.001) as well as upstream or downstream (82%), but few vessels associated with microinfarcts had intact smooth muscle cells (9%).

Interpretation

These observations provide a model for how a single neuropathologic process such as CAA may result in hemorrhagic or ischemic brain lesions potentially through 2 different mechanistic pathways. ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 14, 2019 07:35 PM.

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Targeting microglia using Cx3cr1-cre lines: revisiting the specificity

Microglia play a pivotal role in maintaining homeostasis of the CNS. There is growing interest in understanding how microglia influence normal brain function and disease progression. Several microglia-specific Cx3cr1-Cre lines have been developed and have become indispensable tools in many investigations of microglial function. However, some recent studies have reported that these lines may have significant leakage into neurons. Other studies have reported that Cx3cr1 is expressed in non-microglial cells, including neurons and astrocytes, in vitro or in vivo either during brain development or upon neurological insult. All these reports raise serious concerns about the trustworthiness of these Cre-lines and whether the conclusions drawn from previous studies are valid. Here, we found that a floxed fluorescent reporter mouse line which has been frequently used to verify Cre lines displayed spontaneous expression of the GFP reporter, independent of Cre recombinase, thus revealing a potential caveat in assessing cre lines. We further confirmed that two Cx3cr1-Cre mouse lines can drive fluorescent reporter expression largely restrictively in microglia. Finally, we clarified that these two mouse lines maintain microglia-specific expression even following excitatory injury. Together, our findings confirm that two previously created Cx3cr1-Cre lines remain as invaluable tools for studying microglia. Moreover, to ensure the quality of data generated and the soundness of conclusions drawn from such data, it should be compulsory to thoroughly examine reporter lines for spontaneous leakiness when labeling cells to study CNS function and diseases.

Significance Statement Microglia-specific Cre-lines are essential for studying the role of microglia in the CNS. Several Cx3cr1-Cre lines have been developed and used in a number of landmark studies. However, there is growing concern in the microglia research community regarding potential leakiness of Cre-lines into neurons. The conclusions drawn from previous studies are also being questioned and key ongoing studies have been stalled. We found that a GFP-reporter mouse lines used in a previous study displays spontaneous leakiness into neurons, independent of Cre recombinase. Furthermore, we confirmed that two Cre-lines are microglia-specific and thus can be redeployed without hesitation. Our study also suggests that testing for potential leakiness of GFP-reporter lines should be included as a control in cell-tracing experiments.

in RSS PAP on June 14, 2019 04:30 PM.

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Genetic risk for Alzheimer's disease is distinct from genetic risk for amyloid deposition

Abstract

Objectives

Alzheimer's disease (AD) is the most common form of dementia and is responsible for a huge and growing health care burden in the developed and developing world. The Polygenic Risk Score (PRS) approach has shown 75%‐84% prediction accuracy of identifying individuals with AD risk.

Methods

In this study we tested the prediction accuracy of AD, MCI and amyloid deposition risks with PRS, including and excluding APOE genotypes in a large publicly available data set with extensive phenotypic data: the Alzheimer's Disease Neuroimaging Initiative cohort. Among MCI individuals with amyloid positive status we examined PRS prediction accuracy in those who converted to AD. In addition, we divided polygenic risk score by biological pathways and tested them independently for distinguishing between AD, MCI and amyloid deposition.

Results

We found that AD and MCI are predicted by both APOE genotype and PRS (AUC=0.82% and 68%, respectively). Amyloid deposition is predicted by APOE only (AUC=79%). Further progression to AD of individuals with MCI and amyloid positive status is predicted by PRS over and above APOE (AUC=67%).

In pathway‐specific PRSs analyses the protein‐lipid complex has the strongest association with AD and amyloid deposition even when genes in APOE region were removed (p=0.0055 and p=0.0079, respectively).

Interpretation

The results showed different pattern of APOE contribution in PRS risk predictions of AD/MCI and amyloid deposition. Our study suggests that APOE mostly contributes to amyloid accumulation and the PRS affects risk of further conversion to AD.

This article is protected by copyright. All rights reserved.

in Wiley: Annals of Neurology: Table of Contents on June 14, 2019 02:35 PM.

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Genetic risk for Alzheimer's disease is distinct from genetic risk for amyloid deposition

Abstract

Objectives

Alzheimer's disease (AD) is the most common form of dementia and is responsible for a huge and growing health care burden in the developed and developing world. The Polygenic Risk Score (PRS) approach has shown 75%‐84% prediction accuracy of identifying individuals with AD risk.

Methods

In this study we tested the prediction accuracy of AD, MCI and amyloid deposition risks with PRS, including and excluding APOE genotypes in a large publicly available data set with extensive phenotypic data: the Alzheimer's Disease Neuroimaging Initiative cohort. Among MCI individuals with amyloid positive status we examined PRS prediction accuracy in those who converted to AD. In addition, we divided polygenic risk score by biological pathways and tested them independently for distinguishing between AD, MCI and amyloid deposition.

Results

We found that AD and MCI are predicted by both APOE genotype and PRS (AUC=0.82% and 68%, respectively). Amyloid deposition is predicted by APOE only (AUC=79%). Further progression to AD of individuals with MCI and amyloid positive status is predicted by PRS over and above APOE (AUC=67%).

In pathway‐specific PRSs analyses the protein‐lipid complex has the strongest association with AD and amyloid deposition even when genes in APOE region were removed (p=0.0055 and p=0.0079, respectively).

Interpretation

The results showed different pattern of APOE contribution in PRS risk predictions of AD/MCI and amyloid deposition. Our study suggests that APOE mostly contributes to amyloid accumulation and the PRS affects risk of further conversion to AD.

This article is protected by copyright. All rights reserved.

in Wiley: Annals of Neurology: Table of Contents on June 14, 2019 02:35 PM.

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Modeling and Interpreting Real-world Human Risk Decision Making with Inverse Reinforcement Learning. (arXiv:1906.05803v1 [cs.LG])

We model human decision-making behaviors in a risk-taking task using inverse reinforcement learning (IRL) for the purposes of understanding real human decision making under risk. To the best of our knowledge, this is the first work applying IRL to reveal the implicit reward function in human risk-taking decision making and to interpret risk-prone and risk-averse decision-making policies. We hypothesize that the state history (e.g. rewards and decisions in previous trials) are related to the human reward function, which leads to risk-averse and risk-prone decisions. We design features that reflect these factors in the reward function of IRL and learn the corresponding weight that is interpretable as the importance of features. The results confirm the sub-optimal risk-related decisions of human-driven by the personalized reward function. In particular, the risk-prone person tends to decide based on the current pump number, while the risk-averse person relies on burst information from the previous trial and the average end status. Our results demonstrate that IRL is an effective tool to model human decision-making behavior, as well as to help interpret the human psychological process in risk decision-making.

in q-bio.NC updates on arXiv.org on June 14, 2019 01:30 AM.

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Self-organized critical balanced networks: a unified framework. (arXiv:1906.05624v1 [nlin.AO])

Asynchronous irregular (AI) and critical states are two competing frameworks proposed to explain spontaneous neuronal activity. Here, we propose a mean-field model with simple stochastic neurons that generalizes the integrate-and-fire network of Brunel (2000). We show that the point with balanced inhibitory/excitatory synaptic weight ratio $g_c \approx 4$ corresponds to a second order absorbing phase transition usual in self-organized critical (SOC) models. At the synaptic balance point $g_c$, the network exhibits power-law neuronal avalanches with the usual exponents, whereas for nonzero external field the system displays the four usual synchronicity states of balanced networks. We add homeostatic inhibition and firing rate adaption and obtain a self-organized quasi-critical balanced state with avalanches and AI-like activity. Our model might explain why different inhibition levels are obtained in different experimental conditions and for different regions of the brain, since at least two dynamical mechanisms are necessary to obtain a truly balanced state, without which the network may hover in different regions of the presented theoretical phase diagram.

in q-bio.NC updates on arXiv.org on June 14, 2019 01:30 AM.

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Information capacity of a network of spiking neurons. (arXiv:1906.05584v1 [q-bio.NC])

We study a model of spiking neurons, with recurrent connections that result from learning a set of spatio-temporal patterns with a spike-timing dependent plasticity rule and a global inhibition. We investigate the ability of the network to store and selectively replay multiple patterns of spikes, with a combination of spatial population and phase-of-spike code. Each neuron in a pattern is characterized by a binary variable determining if the neuron is active in the pattern, and a phase-lag variable representing the spike-timing order among the active units. After the learning stage, we study the dynamics of the network induced by a brief cue stimulation, and verify that the network is able to selectively replay the pattern correctly and persistently. We calculate the information capacity of the network, defined as the maximum number of patterns that can be encoded in the network times the number of bits carried by each pattern, normalized by the number of synapses, and find that it can reach a value $\alpha_\text{max}\simeq 0.27$, similar to the one of sequence processing neural networks, and almost double of the capacity of the static Hopfield model. We study the dependence of the capacity on the global inhibition, connection strength (or neuron threshold) and fraction of neurons participating to the patterns. The results show that a dual population and temporal coding can be optimal for the capacity of an associative memory.

in q-bio.NC updates on arXiv.org on June 14, 2019 01:30 AM.

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Modeling functional resting-state brain networks through neural message passing on the human connectome. (arXiv:1906.05369v1 [q-bio.NC])

Understanding the relationship between the structure and function of the human brain is one of the most important open questions in Neurosciences. In particular, Resting State Networks (RSN) and more specifically the Default Mode Network (DMN) of the brain, which are defined from the analysis of functional data lack a definitive justification consistent with the anatomical structure of the brain. In this work, we show that a possible connection may naturally rest on the idea that information flows in the brain through a neural message-passing dynamics between macroscopic structures, like those defined by the human connectome (HC). In our model, each brain region in the HC is assumed to have a binary behavior (active or not), the strength of interactions among them is encoded in the anatomical connectivity matrix defined by the HC, and the dynamics of the system is defined by a neural message-passing algorithm, Belief Propagation (BP), working near the critical point of the human connectome. We show that in the absence of direct external stimuli the BP algorithm converges to a spatial map of activations that is similar to the DMN. Moreover, we computed, using Susceptibility Propagation (SP), the matrix of correlations between the different regions and show that the modules defined by a clustering of this matrix resemble several Resting States Networks determined experimentally. Both results suggest that the functional DMN and RSNs can be seen as simple consequences of the anatomical structure of the brain and a neural message-passing dynamics between macroscopic regions. We then show preliminary results indicating our predictions on how functional DMN maps change when the anatomical brain network suffers structural anomalies, like in Alzheimers Disease and in lesions of the Corpus Callosum.

in q-bio.NC updates on arXiv.org on June 14, 2019 01:30 AM.

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Mice keep their cool

Nature Reviews Neuroscience, Published online: 14 June 2019; doi:10.1038/s41583-019-0198-1

in Nature Reviews Neuroscience - Issue - nature.com science feeds on June 14, 2019 12:00 AM.

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Interspecies Differences in the Connectivity of Ventral Striatal Components Between Humans and Macaques

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 14, 2019 12:00 AM.

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The Age-Related Central Auditory Processing Disorder: Silent Impairment of the Cognitive Ear

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 14, 2019 12:00 AM.

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Brain Molecular Connectivity in Neurodegenerative Diseases: Recent Advances and New Perspectives Using Positron Emission Tomography

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 14, 2019 12:00 AM.

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L-Dopa Modulation of Brain Connectivity in Parkinson’s Disease Patients: A Pilot EEG-fMRI Study

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 14, 2019 12:00 AM.

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Hybrid Functional Brain Network With First-Order and Second-Order Information for Computer-Aided Diagnosis of Schizophrenia

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 14, 2019 12:00 AM.

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Mechanics of Brain Tissues Studied by Atomic Force Microscopy: A Perspective

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on June 14, 2019 12:00 AM.

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Effect of L-DOPA/Benserazide on Propagation of Pathological α-Synuclein

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 14, 2019 12:00 AM.

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The Dual Role of AQP4 in Cytotoxic and Vasogenic Edema Following Spinal Cord Contusion and Its Possible Association With Energy Metabolism via COX5A

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 14, 2019 12:00 AM.

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Semantic Processing in Bilingual Aphasia: Evidence of Language Dependency

in Frontiers in Human Neuroscience | New and Recent Articles on June 14, 2019 12:00 AM.

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Characterizing and Predicting Autism Spectrum Disorder by Performing Resting-State Functional Network Community Pattern Analysis

in Frontiers in Human Neuroscience | New and Recent Articles on June 14, 2019 12:00 AM.

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Decoding P300 Variability Using Convolutional Neural Networks

in Frontiers in Human Neuroscience | New and Recent Articles on June 14, 2019 12:00 AM.

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Are we there yet?

in eLife: latest articles on June 14, 2019 12:00 AM.

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Integrative modeling of the HIV-1 ribonucleoprotein complex

by David S. Goodsell, Andrew Jewett, Arthur J. Olson, Stefano Forli

in PLOS Computational Biology: New Articles on June 13, 2019 09:00 PM.

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Correction: Atrial arrhythmogenicity of <i>KCNJ2</i> mutations in short QT syndrome: Insights from virtual human atria

by The PLOS Computational Biology Staff

in PLOS Computational Biology: New Articles on June 13, 2019 09:00 PM.

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Development of a physiologically-based pharmacokinetic pediatric brain model for prediction of cerebrospinal fluid drug concentrations and the influence of meningitis

by Laurens F. M. Verscheijden, Jan B. Koenderink, Saskia N. de Wildt, Frans G. M. Russel

in PLOS Computational Biology: New Articles on June 13, 2019 09:00 PM.

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Disentangling juxtacrine from paracrine signalling in dynamic tissue

by Hiroshi Momiji, Kirsty L. Hassall, Karen Featherstone, Anne V. McNamara, Amanda L. Patist, David G. Spiller, Helen C. Christian, Michael R. H. White, Julian R. E. Davis, Bärbel F. Finkenstädt, David A. Rand

in PLOS Computational Biology: New Articles on June 13, 2019 09:00 PM.

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Fostering bioinformatics education through skill development of professors: <i>Big Genomic Data Skills Training for Professors</i>

by Yingqian Ada Zhan, Charles Gregory Wray, Sandeep Namburi, Spencer T. Glantz, Reinhard Laubenbacher, Jeffrey H. Chuang

in PLOS Computational Biology: New Articles on June 13, 2019 09:00 PM.

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Dynamic brain interactions during picture naming

Brain computations involve multiple processes by which sensory information is encoded and transformed to drive behavior. These computations are thought to be mediated by dynamic interactions between populations of neurons. Here we demonstrate that human brains exhibit a reliable sequence of neural interactions during speech production. We use an autoregressive hidden Markov model to identify dynamical network states exhibited by electrocorticographic signals recorded from human neurosurgical patients. Our method resolves dynamic latent network states on a trial-by-trial basis. We characterize individual network states according to the patterns of directional information flow between cortical regions of interest. These network states occur consistently and in a specific, interpretable sequence across trials and subjects: the data support the hypothesis of a fixed-length visual processing state, followed by a variable-length language state, and then by a terminal articulation state. This empirical evidence validates classical psycho-linguistic theories that have posited such intermediate states during speaking. It further reveals these state dynamics are not localized to one brain area or one sequence of areas, but are instead a network phenomenon.

Significance Cued speech production engages a distributed set of brain regions that must interact with each other to perform this behavior rapidly and precisely. To characterize the spatio-temporal properties of the networks engaged in picture naming, we recorded from electrodes placed directly on the brain surfaces of patients with epilepsy being evaluated for surgical resection. We used a flexible statistical model applied to broadband gamma to characterize changing brain interactions. Unlike conventional models, ours can identify changes on individual trials that correlate with behavior. Our results reveal that interactions between brain regions are consistent across trials. This flexible statistical model provides a useful platform for quantifying brain dynamics during cognitive processes.

in RSS PAP on June 13, 2019 04:30 PM.

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Issue Information

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Annals of Neurology: Volume 86, Number 1, July 2019

A fluorescence photomicrograph showing the localization of JBTS17, a protein that organizes microtubules during cell division and which is mutated in Joubert syndrome. The nucleus of the cell is stained blue, the microtubules red and JBTS17 green. Note the localization of JBTS17 along the nuclear envelope and in the cytoplasm along microtubules. See Hong et al., pp. 99–115 for details.

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Electroencephalographic reactivity as predictor of neurological outcome in postanoxic coma: A multicenter prospective cohort study

Objective

Outcome prediction in patients after cardiac arrest (CA) is challenging. Electroencephalographic reactivity (EEG‐R) might be a reliable predictor. We aimed to determine the prognostic value of EEG‐R using a standardized assessment.

Methods

In a prospective cohort study, a strictly defined EEG‐R assessment protocol was executed twice per day in adult patients after CA. EEG‐R was classified as present or absent by 3 EEG readers, blinded to patient characteristics. Uncertain reactivity was classified as present. Primary outcome was best Cerebral Performance Category score (CPC) in 6 months after CA, dichotomized as good (CPC = 1–2) or poor (CPC = 3–5). EEG‐R was considered reliable for predicting poor outcome if specificity was ≥95%. For good outcome prediction, a specificity of ≥80% was used. Added value of EEG‐R was the increase in specificity when combined with EEG background, neurological examination, and somatosensory evoked potentials (SSEPs).

Results

Of 160 patients enrolled, 149 were available for analyses. Absence of EEG‐R for poor outcome prediction had a specificity of 82% and a sensitivity of 73%. For good outcome prediction, specificity was 73% and sensitivity 82%. Specificity for poor outcome prediction increased from 98% to 99% when EEG‐R was added to a multimodal model. For good outcome prediction, specificity increased from 70% to 89%.

Interpretation

EEG‐R testing in itself is not sufficiently reliable for outcome prediction in patients after CA. For poor outcome prediction, it has no substantial added value to EEG background, neurological examination, and SSEPs. For prediction of good outcome, EEG‐R seems to have added value. ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Residual descending motor pathways influence spasticity after spinal cord injury

Objective

Spasticity is one of the most common symptoms manifested in humans with spinal cord injury (SCI). The neural mechanisms contributing to its development are not yet understood. Using neurophysiological and imaging techniques, we examined the influence of residual descending motor pathways on spasticity in humans with SCI.

Methods

We measured spasticity in 33 individuals with motor complete SCI (determined by clinical examination) without preservation of voluntary motor output in the quadriceps femoris muscle. To examine residual descending motor pathways, we used magnetic and electrical stimulation over the leg motor cortex to elicit motor evoked potentials (MEPs) in the quadriceps femoris muscle and structural magnetic resonance imaging to measure spinal cord atrophy.

Results

We found that 60% of participants showed symptoms of spasticity, whereas the other 40% showed no spasticity, demonstrating the presence of 2 clear subgroups of humans with motor complete SCI. MEPs were only present in individuals who had spasticity, and MEP size correlated with the severity of spasticity. Spinal cord atrophy was greater in nonspastic compared with spastic subjects. Notably, the degree of spared tissue in the lateral regions of the spinal cord was positively correlated with the severity of spasticity, indicating preservation of white matter related to motor tracts when spasticity was present.

Interpretation

These results support the hypothesis that preservation of descending motor pathways influences spasticity in humans with motor complete SCI; this knowledge might help the rehabilitation and assessment of people with SCI. ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Glial injury in neurotoxicity after pediatric CD19‐directed chimeric antigen receptor T cell therapy

Objective

To test whether systemic cytokine release is associated with central nervous system inflammatory responses and glial injury in immune effector cell‐associated neurotoxicity syndrome (ICANS) after chimeric antigen receptor (CAR)‐T cell therapy in children and young adults.

Methods

We performed a prospective cohort study of clinical manifestations as well as imaging, pathology, CSF, and blood biomarkers on 43 subjects ages 1 to 25 who received CD19‐directed CAR/T cells for acute lymphoblastic leukemia (ALL).

Results

Neurotoxicity occurred in 19 of 43 (44%) subjects. Nine subjects (21%) had CTCAE grade 3 or 4 neurological symptoms, with no neurotoxicity‐related deaths. Reversible delirium, headache, decreased level of consciousness, tremor, and seizures were most commonly observed. Cornell Assessment of Pediatric Delirium (CAPD) scores ≥9 had 94% sensitivity and 33% specificity for grade ≥3 neurotoxicity, and 91% sensitivity and 72% specificity for grade ≥2 neurotoxicity. Neurotoxicity correlated with severity of cytokine release syndrome, abnormal past brain magnetic resonance imaging (MRI), and higher peak CAR‐T cell numbers in blood, but not cerebrospinal fluid (CSF). CSF levels of S100 calcium‐binding protein B and glial fibrillary acidic protein increased during neurotoxicity, indicating astrocyte injury. There were concomitant increases in CSF white blood cells, protein, interferon‐γ (IFNγ), interleukin (IL)‐6, IL‐10, and granzyme B (GzB), with concurrent elevation of serum IFNγ IL‐10, GzB, granulocyte macrophage colony‐stimulating factor, macrophage inflammatory protein 1 alpha, and tumor necrosis factor alpha, but not IL‐6. We did not find direct evidence of endothelial activation.

Interpretation

Our data are most consistent with ICANS as a syndrome of systemic inflammation, which affects the brain through compromise of the neurovascular unit and astrocyte injury. ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Genetic risk of dementia mitigated by cognitive reserve: A cohort study

Objective

We investigated whether cognitive reserve modifies the risk of dementia attributable to apolipoprotein ε4 (APOE‐ε4), a well‐known genetic risk factor for dementia.

Methods

We followed 2,556 cognitively intact participants aged ≥60 years from the ongoing prospective community‐based Swedish National Study on Aging and Care in Kungsholmen (SNAC‐K). Dementia was ascertained through clinical and neuropsychological assessments and diagnosed according to Diagnostic and Statistical Manual of Mental Disorders, 4th edition criteria. Structural equation modeling was used to generate a cognitive reserve indicator from 4 previously validated contributors: early life education, midlife substantive work complexity, late life leisure activities, and late life social networks. Cox proportional hazard models estimated dementia risk in relation to cognitive reserve indicator. The interaction between the cognitive reserve indicator and APOE‐ε4 was assessed on multiplicative and additive scales.

Results

After an average of 6.3 years (range = 2.1–10.7) of follow‐up, 232 dementia cases were ascertained. Relative to individuals in the lowest tertile of cognitive reserve indicator, those with moderate and high reserve were at a reduced risk of dementia. There was no multiplicative interaction between APOE‐ε4 status and cognitive reserve indicator (p = 0.113). Additive interaction was statistically significant. Relative to APOE‐ε4 carriers with low cognitive reserve, ε4 carriers with high reserve had a reduced risk of dementia (hazard ratio [HR] = 0.28, 95% confidence interval [CI] = 0.13–0.59). The magnitude of risk reduction was similar in ε4 noncarriers with a high cognitive reserve indicator (HR = 0.24, 95% CI = 0.15–0.40).

Interpretation

Lifelong engagement in reserve‐enhancing activities attenuates the risk of dementia attributable to APOE‐ε4. Promoting cognitive reserve might be especially effective in subpopulations with high genetic risk of dementia. ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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A multicenter retrospective study of charcot‐marie‐tooth disease type 4B (CMT4B) associated with mutations in myotubularin‐related proteins (MTMRs)

Objective

Charcot‐Marie‐Tooth (CMT) disease 4B1 and 4B2 (CMT4B1/B2) are characterized by recessive inheritance, early onset, severe course, slowed nerve conduction, and myelin outfoldings. CMT4B3 shows a more heterogeneous phenotype. All are associated with myotubularin‐related protein (MTMR) mutations. We conducted a multicenter, retrospective study to better characterize CMT4B.

Methods

We collected clinical and genetic data from CMT4B subjects in 18 centers using a predefined minimal data set including Medical Research Council (MRC) scores of nine muscle pairs and CMT Neuropathy Score.

Results

There were 50 patients, 21 of whom never reported before, carrying 44 mutations, of which 21 were novel and six representing novel disease associations of known rare variants. CMT4B1 patients had significantly more‐severe disease than CMT4B2, with earlier onset, more‐frequent motor milestones delay, wheelchair use, and respiratory involvement as well as worse MRC scores and motor CMT Examination Score components despite younger age at examination. Vocal cord involvement was common in both subtypes, whereas glaucoma occurred in CMT4B2 only. Nerve conduction velocities were similarly slowed in both subtypes. Regression analyses showed that disease severity is significantly associated with age in CMT4B1. Slopes are steeper for CMT4B1, indicating faster disease progression. Almost none of the mutations in the MTMR2 and MTMR13 genes, responsible for CMT4B1 and B2, respectively, influence the correlation between disease severity and age, in agreement with the hypothesis of a complete loss of function of MTMR2/13 proteins for such mutations.

Interpretation

This is the largest CMT4B series ever reported, demonstrating that CMT4B1 is significantly more severe than CMT4B2, and allowing an estimate of prognosis. ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Epilepsy in families: Age at onset is a familial trait, independent of syndrome

Objective

We tested 2 hypotheses regarding age at onset within familial epilepsies: (1) family members with epilepsy tend to have similar ages at onset, independent of epilepsy syndrome; and (2) age at onset is younger in successive generations after controlling for sampling bias.

Methods

We analyzed clinical data collected by the Epi4K Consortium (303 multiplex families, 1,120 individuals). To test hypothesis 1, we used both linear mixed models commonly used for heritability analysis and Cox regression models with frailty terms to assess clustering of onset within families after controlling for other predictors. To test hypothesis 2, we used mixed effects models, pairwise analyses, and survival analysis to address sampling‐related bias that may mimic anticipation.

Results

Regarding hypothesis 1, age at seizure onset was significantly heritable (intraclass correlation coefficient = 0.17, p < 0.001) after adjusting for epilepsy type, sex, site, history of febrile seizure, and age at last observation. This finding remained significant after adjusting for epilepsy syndromes, and was robust across statistical methods in all families and in generalized families. Regarding hypothesis 2, the mean age at onset decreased in successive generations (p < 0.001). After adjusting for age at last observation, this effect was not significant in mixed effects models (p = 0.14), but remained significant in pairwise (p = 0.0003) and survival analyses (p = 0.02).

Interpretation

Age at seizure onset is an independent familial trait, and may have genetic determinants distinct from the determinants of particular epilepsy syndromes. Younger onsets in successive generations can be explained in part by sampling bias, but the presence of genetic anticipation cannot be excluded. ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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The Effect of Intrathecal Baclofen in Dyskinetic Cerebral Palsy: The IDYS Trial

Objective

Intrathecal baclofen treatment is used for the treatment of dystonia in patients with severe dyskinetic cerebral palsy; however, the current level of evidence for the effect is low. The primary aim of this study was to provide evidence for the effect of intrathecal baclofen treatment on individual goals in patients with severe dyskinetic cerebral palsy.

Methods

This multicenter, randomized, double‐blind, placebo‐controlled trial was performed at 2 university medical centers in the Netherlands. Patients with severe dyskinetic cerebral palsy (Gross Motor Functioning Classification System level IV–V) aged 4 to 24 years who were eligible for intrathecal baclofen were included. Patients were assigned by block randomization (2:2) for treatment with intrathecal baclofen or placebo for 3 months via an implanted microinfusion pump. The primary outcome was goal attainment scaling of individual treatment goals (GAS T score). A linear regression model was used for statistical analysis with study site as a covariate. Safety analyses were done for number and type of (serious) adverse events.

Results

Thirty‐six patients were recruited from January 1, 2013, to March 31, 2018. Data for final analysis were available for 17 patients in the intrathecal baclofen group and 16 in the placebo group. Mean (standard deviation) GAS T score at 3 months was 38.9 (13.2) for intrathecal baclofen and 21.0 (4.6) for placebo (regression coefficient = 17.8, 95% confidence interval = 10.4‐25.0, p < 0.001). Number and types of (serious) adverse events were similar between groups.

Interpretation

Intrathecal baclofen treatment is superior to placebo in achieving treatment goals in patients with severe dyskinetic cerebral palsy. ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Reply to “Grading the severity of autoimmune encephalitis: Advances and pitfalls”

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Grading the severity of autoimmune encephalitis: Advances and pitfalls

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Histological features of intracranial thrombi in stroke patients with cancer

The histological features of thrombus in stroke patients with cancer are not well known. Using immunohistochemical staining of thrombi retrieved during mechanical thrombectomy in stroke patients, thrombus compositions were compared between 16 patients with active cancer, 16 patients with inactive cancer, and 16 patients without any history of cancer. The active cancer group showed higher platelet and lower erythrocyte fractions than the inactive cancer or the control group. Four patients with vegetation showed very high platelet and low erythrocyte fractions. Patients with cryptogenic etiology in the active cancer group showed a similar pattern to those with vegetation. These findings may aid the determination of treatment strategies in cancer‐associated stroke. ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Novel mutations in MYBPC1 are associated with myogenic tremor and mild myopathy

Objective

To define a distinct, dominantly inherited, mild skeletal myopathy associated with prominent and consistent tremor in two unrelated, three‐generation families.

Methods

Clinical evaluations as well as exome and panel sequencing analyses were performed in affected and nonaffected members of two families to identify genetic variants segregating with the phenotype. Histological assessment of a muscle biopsy specimen was performed in 1 patient, and quantitative tremor analysis was carried out in 2 patients. Molecular modeling studies and biochemical assays were performed for both mutations.

Results

Two novel missense mutations in MYBPC1 (p.E248K in family 1 and p.Y247H in family 2) were identified and shown to segregate perfectly with the myopathy/tremor phenotype in the respective families. MYBPC1 encodes slow myosin binding protein‐C (sMyBP‐C), a modular sarcomeric protein playing structural and regulatory roles through its dynamic interaction with actin and myosin filaments. The Y247H and E248K mutations are located in the NH₂‐terminal M‐motif of sMyBP‐C. Both mutations result in markedly increased binding of the NH₂ terminus to myosin, possibly interfering with normal cross‐bridge cycling as the first muscle‐based step in tremor genesis. The clinical tremor features observed in all mutation carriers, together with the tremor physiology studies performed in family 2, suggest amplification by an additional central loop modulating the clinical tremor phenomenology.

Interpretation

Here, we link two novel missense mutations in MYBPC1 with a dominant, mild skeletal myopathy invariably associated with a distinctive tremor. The molecular, genetic, and clinical studies are consistent with a unique sarcomeric origin of the tremor, which we classify as “myogenic tremor.” ANN NEUROL 2019

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Cell therapy for ischemic stroke: Are differences in preclinical and clinical study design responsible for the translational loss of efficacy?

in Wiley: Annals of Neurology: Table of Contents on June 13, 2019 10:45 AM.

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Hysteresis, neural avalanches and critical behaviour near a first-order transition of a spiking neural network. (arXiv:1906.05166v1 [q-bio.NC])

Many experimental results, both in-vivo and in-vitro, support the idea that the brain cortex operates near a critical point, and at the same time works as a reservoir of precise spatio-temporal patterns. However the mechanism at the basis of these observations is still not clear. In this paper we introduce a model which combines both these features, showing that scale-free avalanches are the signature of a system posed near the spinodal line of a first order transition, with many spatio-temporal patterns stored as dynamical metastable attractors. Specifically, we studied a network of leaky integrate and fire neurons, whose connections are the result of the learning of multiple spatio-temporal dynamical patterns, each with a randomly chosen ordering of the neurons. We found that the network shows a first order transition between a low spiking rate disordered state (down), and a high rate state characterized by the emergence of collective activity and the replay of one of the stored patterns (up). The transition is characterized by hysteresis, or alternation of up and down states, depending on the lifetime of the metastable states. In both cases, critical features and neural avalanches are observed. Notably, critical phenomena occur at the edge of a discontinuous phase transition, as recently observed in a network of glow lamps.

in q-bio.NC updates on arXiv.org on June 13, 2019 01:30 AM.

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Author Correction: Control of tumor-associated macrophages and T cells in glioblastoma via AHR and CD39

Nature Neuroscience, Published online: 13 June 2019; doi:10.1038/s41593-019-0446-8

in Nature Neuroscience - Issue - nature.com science feeds on June 13, 2019 12:00 AM.

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Metabolism of Stem and Progenitor Cells: Proper Methods to Answer Specific Questions

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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Lack of Fractalkine Receptor on Macrophages Impairs Spontaneous Recovery of Ribbon Synapses After Moderate Noise Trauma in C57BL/6 Mice

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 13, 2019 12:00 AM.

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Editorial: Spatial Navigation: Memory Mechanisms and Executive Function Interactions

in Frontiers in Human Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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Functional Spectroscopy Mapping of Pain Processing Cortical Areas During Non-painful Peripheral Electrical Stimulation of the Accessory Spinal Nerve

in Frontiers in Human Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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Links Between the Amplitude Modulation of Low-Frequency Spontaneous Fluctuation Across Resting State Conditions and Thalamic Functional Connectivity

in Frontiers in Human Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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Modulation of Fronto-Striatal Functional Connectivity Using Transcranial Magnetic Stimulation

in Frontiers in Human Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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Intrinsic Spine Dynamics Are Critical for Recurrent Network Learning in Models With and Without Autism Spectrum Disorder

in Frontiers in Computational Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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Transient Potassium Channels: Therapeutic Targets for Brain Disorders

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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Neuroinflammation and Glial Phenotypic Changes in Alpha-Synucleinopathies

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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17β-Estradiol Treatment Attenuates Neurogenesis Damage and Improves Behavior Performance After Ketamine Exposure in Neonatal Rats

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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Hippocampal Sequences During Exploration: Mechanisms and Functions

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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Involvement of microRNA-34a in Age-Related Susceptibility to Oxidative Stress in ARPE-19 Cells by Targeting the Silent Mating Type Information Regulation 2 Homolog 1/p66shc Pathway: Implications for Age-Related Macular Degeneration

in Frontiers in Aging Neuroscience | New and Recent Articles on June 13, 2019 12:00 AM.

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A Discrete Dorsal Raphe to Basal Amygdala 5-HT Circuit Calibrates Aversive Memory

in Neuron on June 13, 2019 12:00 AM.

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A Specialized Neural Circuit Gates Social Vocalizations in the Mouse

in Neuron on June 13, 2019 12:00 AM.

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A roadmap for understanding memory: Decomposing cognitive processes into operations and representations

Thanks to patients Phineas Gage and Henry Molaison, we have long known that behavioral control depends on the frontal lobes, whereas declarative memory depends on the medial temporal lobes (MTL). For decades, cognitive functions – behavioral control, declarative memory – have served as labels for characterizing the division of labor in cortex. This approach has made enormous contributions to understanding how the brain enables the mind, providing a systems-level explanation of brain function that constrains lower-level investigations of neural mechanism. Today, the approach has evolved such that functional labels are often applied to brain networks rather than focal brain regions. Furthermore, the labels have diversified to include both broadly-defined cognitive functions (declarative memory, visual perception) and more circumscribed mental processes (recollection, familiarity, priming). We ask whether a process – a high-level mental phenomenon corresponding to an introspectively-identifiable cognitive event – is the most productive label for dissecting memory. For example, recollection conflates a neurocomputational operation (pattern completion-based retrieval) with a class of representational content (associative, high-dimensional memories). Because a full theory of memory must identify operations and representations separately, and specify how they interact, we argue that processes like recollection constitute inadequate labels for characterizing neural mechanisms. Instead, we advocate considering the component operations and representations of processes like recollection in isolation. For the organization of memory, the evidence suggests that pattern completion is recapitulated widely across the ventral visual stream and MTL, but the division of labor between sites within this pathway can be explained by representational content.

Significance Statement Accounts of cognition often assume that the brain is organized along lines of cognitive process, for example, with recollection mediated by one neural structure and familiarity by another. We argue that cognitive processes – introspectively-identifiable mental events like recollection – are inadequate labels for characterizing neural mechanisms, because they conflate lower-level components of the mechanisms we seek to identify. Recollection involves both a neurocomputational operation (pattern completion) and a neural representation (high-dimensional, associative content). To uncover memory's mechanisms, we must decompose memory processes into their operations and representations, asking how each contributes to mnemonic phenomena. Decomposing recollection suggests that, within the ventral visual pathway and MTL, different brain regions contribute to memory retrieval according to their representational content.

in RSS PAP on June 12, 2019 05:42 PM.

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Spontaneous Recurrent Absence Seizure-like Events in Wild-Caught Rats

Absence epilepsy is a heritable human neurological disorder characterized by brief nonconvulsive seizures with behavioral arrest, moderate-to-severe loss of consciousness (absence), and distinct spike-wave discharges (SWDs) in the EEG and electrocorticogram (ECoG). Genetic models of this disorder have been created by selectively inbreeding rats for absence seizure-like events with similar electrical and behavioral characteristics. However, these events are also common in outbred laboratory rats, raising concerns about whether SWD/immobility accurately reflects absence epilepsy as opposed to "normal" rodent behavior. We hypothesized that, if SWD/immobility models absence seizures, it would not exist in wild-caught rats due to the pressures of natural selection. To test this hypothesis, we compared chronic video/electrocorticogram recordings from male and female wild-caught (Brown-Norway [BN]) rats to recordings from laboratory outbred BN, outbred Long–Evans, and inbred WAG/Rij rats (i.e., a model of absence epilepsy). Wild-caught BN rats displayed absence-like SWD/immobility events that were highly similar to outbred BN rats in terms of spike-wave morphology, frequency, diurnal rhythmicity, associated immobility, and sensitivity to the anti-absence drug, ethosuximide; however, SWD bursts were less frequent and of shorter duration in wild-caught and outbred BN rats than the outbred Long–Evans and inbred WAG/Rij strains. We conclude that SWD/immobility in rats does not represent absence seizures, although they appear to have many similarities. In wild rats, SWD/immobility appears to represent normal brain activity that does not reduce survival in natural environments, a conclusion that logically extends to outbred laboratory rats and possibly to those that have been inbred to model absence epilepsy.

SIGNIFICANCE STATEMENT Spike-wave discharges (SWDs), behavioral arrest, and diminished consciousness are cardinal signs of seizures in human absence epilepsy and are used to model this disorder in inbred rats. These characteristics, however, are routinely found in outbred laboratory rats, leading to debate on whether SWD/immobility is a valid model of absence seizures. The SWD/immobility events in wild-caught rats appear equivalent to those found in outbred and inbred rat strains, except for lower incidence and shorter durations. Our results indicate that the electrophysiological and behavioral characteristics of events underlying hypothetical absence epilepsy in rodent models are found in wild rats captured in their natural environment. Other criteria beyond observation of SWDs and associated immobility are required to objectively establish absence epilepsy in rat models.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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AMPA Receptor Dysregulation and Therapeutic Interventions in a Mouse Model of CDKL5 Deficiency Disorder

Pathogenic mutations in cyclin-dependent kinase-like 5 (CDKL5) result in CDKL5 deficiency disorder (CDD), a rare disease marked by early-life seizures, autistic behaviors, and intellectual disability. Although mouse models of CDD exhibit dendritic instability and alterations in synaptic scaffolding proteins, studies of glutamate receptor levels and function are limited. Here we used a novel mouse model of CDD, the Cdkl5^R59X knock-in mouse (R59X), to investigate changes in synaptic glutamate receptor subunits and functional consequences. Male mice were used for all experiments to avoid the confounding effects of X-inactivation that would be present in female heterozygous mice. We showed that adult male R59X mice recapitulated the behavioral outcomes observed in other mouse models of CDD, including social deficits and memory and learning impairments, and exhibited decreased latency to seizure upon pentylenetetrazol administration. Furthermore, we observed a specific increase in GluA2-lacking α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid)-type glutamate receptors (AMPARs) in the adult R59X hippocampus, which is accompanied electrophysiologically by increased rectification ratio of AMPAR EPSCs and elevated early-phase long term potentiation (LTP). Finally, we showed that acute treatment with the GluA2-lacking AMPAR blocker IEM-1460 decreased AMPAR currents, and rescued social deficits, working memory impairments, and seizure behavior latency in R59X mice.

SIGNIFICANCE STATEMENT CDKL5 deficiency disorder (CDD) is a rare disease marked by autistic-like behaviors, intellectual disability, and seizures. While synaptic dysfunction has been observed in mouse models of CDD, there is limited information on how synaptic alterations contribute to behavioral and functional changes in CDD. Here we reveal elevated hippocampal GluA2-lacking AMPAR expression in a novel mouse model of CDD that is accompanied by changes in synaptic AMPAR function and plasticity. We also show, for the first time, that acutely targeting GluA2-lacking AMPAR dysregulation rescues core synaptic and neurobehavioral deficits in CDD.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Modulators of Kv3 Potassium Channels Rescue the Auditory Function of Fragile X Mice

Fragile X syndrome (FXS) is characterized by hypersensitivity to sensory stimuli, including environmental sounds. We compared the auditory brainstem response (ABR) recorded in vivo in mice lacking the gene (Fmr1^–/y) for fragile X mental retardation protein (FMRP) with that in wild-type animals. We found that ABR wave I, which represents input from the auditory nerve, is reduced in Fmr1^–/y animals, but only at high sound levels. In contrast, wave IV, which represents the activity of auditory brainstem nuclei is enhanced at all sound levels, suggesting that loss of FMRP alters the central processing of auditory signals. Current-clamp recordings of neurons in the medial nucleus of the trapezoid body in the auditory brainstem revealed that, in contrast to neurons from wild-type animals, sustained depolarization triggers repetitive firing rather than a single action potential. In voltage-clamp recordings, K⁺ currents that activate at positive potentials ("high-threshold" K⁺ currents), which are required for high-frequency firing and are carried primarily by Kv3.1 channels, are elevated in Fmr1^–/y mice, while K⁺ currents that activate near the resting potential and inhibit repetitive firing are reduced. We therefore tested the effects of AUT2 [((4-({5-[(4R)-4-ethyl-2,5-dioxo-1-imidazolidinyl]-2-pyridinyl}oxy)-2-(1-methylethyl) benzonitrile], a compound that modulates Kv3.1 channels. AUT2 reduced the high-threshold K⁺ current and increased the low-threshold K⁺ currents in neurons from Fmr1^–/y animals by shifting the activation of the high-threshold current to more negative potentials. This reduced the firing rate and, in vivo, restored wave IV of the ABR. Our results from animals of both sexes suggest that the modulation of the Kv3.1 channel may have potential for the treatment of sensory hypersensitivity in patients with FXS.

SIGNIFICANCE STATEMENT mRNA encoding the Kv3.1 potassium channel was one of the first described targets of the fragile X mental retardation protein (FMRP). Fragile X syndrome is caused by loss of FMRP and, in humans and mice, causes hypersensitivity to auditory stimuli. We found that components of the auditory brain response (ABR) corresponding to auditory brainstem activity are enhanced in mice lacking FMRP. This is accompanied by hyperexcitability and altered potassium currents in auditory brainstem neurons. Treatment with a drug that alters the voltage dependence of Kv3.1 channels normalizes the imbalance of potassium currents, as well as ABR responses in vivo, suggesting that such compounds may be effective in treating some symptoms of fragile X syndrome.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Synaptic Depotentiation and mGluR5 Activity in the Nucleus Accumbens Drive Cocaine-Primed Reinstatement of Place Preference

Understanding the neurobiological processes that incite drug craving and drive relapse has the potential to help target efforts to treat addiction. The NAc serves as a critical substrate for reward and motivated behavior, in part due to alterations in excitatory synaptic strength within cortical-accumbens pathways. The present studies investigated a causal link between cocaine-induced reinstatement of conditioned place preference and rapid reductions of cocaine-dependent increases in NAc shell synaptic strength in male mice. Cocaine-conditioned place preference behavior and ex vivo whole-cell electrophysiology showed that cocaine-primed reinstatement and synaptic depotentiation were disrupted by inhibiting AMPAR internalization via intra-NAc shell infusion of a Tat-GluA2_3Y peptide. Furthermore, reinstatement was driven by an mGluR5-dependent reduction in AMPAR signaling. Intra-NAc shell infusion of the mGluR5 antagonist MTEP blocked cocaine-primed reinstatement and corresponding depotentiation, whereas infusion of the mGluR5 agonist CHPG itself promoted reinstatement and depotentiated synaptic strength in the NAc shell. Optogenetic examination of circuit-specific plasticity showed that inhibition of infralimbic cortical input to the NAc shell blocked cocaine-primed reinstatement, whereas low-frequency stimulation (10 Hz) of this pathway in the absence of cocaine triggered a reduction in synaptic strength akin to that observed with cocaine, and was sufficient to promote reinstatement in the absence of a cocaine challenge. These data support a model in which mGluR5-mediated reduction in GluA2-containing AMPARs at NAc shell synapses receiving input from the infralimbic cortex is a critical factor in triggering reinstatement of cocaine-primed conditioned approach behavior.

SIGNIFICANCE STATEMENT These studies identified a sequence of neural events whereby reexposure to cocaine activates a signaling cascade that alters synaptic strength in the NAc shell and triggers a behavioral response driven by a drug-associated memory.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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EEG Frontal Alpha Asymmetry and Dream Affect: Alpha Oscillations over the Right Frontal Cortex during REM Sleep and Presleep Wakefulness Predict Anger in REM Sleep Dreams

Affective experiences are central not only to our waking life but also to rapid eye movement (REM) sleep dreams. Despite our increasing understanding of the neural correlates of dreaming, we know little about the neural correlates of dream affect. Frontal alpha asymmetry (FAA) is considered a marker of affective states and traits as well as affect regulation in the waking state. Here, we explored whether FAA during REM sleep and during evening resting wakefulness is related to affective experiences in REM sleep dreams. EEG recordings were obtained from 17 human participants (7 men) who spent 2 nights in the sleep laboratory. Participants were awakened 5 min after the onset of every REM stage after which they provided a dream report and rated their dream affect. Two-minute preawakening EEG segments were analyzed. Additionally, 8 min of evening presleep and morning postsleep EEG were recorded during resting wakefulness. Mean spectral power in the alpha band (8–13 Hz) and corresponding FAA were calculated over the frontal (F4-F3) sites. Results showed that FAA during REM sleep, and during evening resting wakefulness, predicted ratings of dream anger. This suggests that individuals with greater alpha power in the right frontal hemisphere may be less able to regulate (i.e., inhibit) strong affective states, such as anger, in dreams. Additionally, FAA was positively correlated across wakefulness and REM sleep. Together, these findings imply that FAA may serve as a neural correlate of affect regulation not only in the waking but also in the dreaming state.

SIGNIFICANCE STATEMENT We experience emotions not only during wakefulness but also during dreaming. Despite our increasing understanding of the neural correlates of dreaming, we know little about the neural correlates of dream emotions. Here we used electroencephalography to explore how frontal alpha asymmetry (FAA)—the relative difference in alpha power between the right and left frontal cortical areas that is associated with emotional processing and emotion regulation in wakefulness—is related to dream emotions. We show that individuals with greater FAA (i.e., greater right-sided alpha power) during rapid eye movement sleep, and during evening wakefulness, experience more anger in dreams. FAA may thus reflect the ability to regulate emotions not only in the waking but also in the dreaming state.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Neural Coding for Shape and Texture in Macaque Area V4

The distinct visual sensations of shape and texture have been studied separately in cortex; therefore, it remains unknown whether separate neuronal populations encode each of these properties or one population carries a joint encoding. We directly compared shape and texture selectivity of individual V4 neurons in awake macaques (1 male, 1 female) and found that V4 neurons lie along a continuum from strong tuning for boundary curvature of shapes to strong tuning for perceptual dimensions of texture. Among neurons tuned to both attributes, tuning for shape and texture were largely separable, with the latter delayed by ~30 ms. We also found that shape stimuli typically evoked stronger, more selective responses than did texture patches, regardless of whether the latter were contained within or extended beyond the receptive field. These results suggest that there are separate specializations in mid-level cortical processing for visual attributes of shape and texture.

SIGNIFICANCE STATEMENT Object recognition depends on our ability to see both the shape of the boundaries of objects and properties of their surfaces. However, neuroscientists have never before examined how shape and texture are linked together in mid-level visual cortex. In this study, we used systematically designed sets of simple shapes and texture patches to probe the responses of individual neurons in the primate visual cortex. Our results provide the first evidence that some cortical neurons specialize in processing shape whereas others specialize in processing textures. Most neurons lie between the ends of this continuum, and in these neurons we find that shape and texture encoding are largely independent.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Single-Cell Membrane Potential Fluctuations Evince Network Scale-Freeness and Quasicriticality

What information single neurons receive about general neural circuit activity is a fundamental question for neuroscience. Somatic membrane potential (V_m) fluctuations are driven by the convergence of synaptic inputs from a diverse cross-section of upstream neurons. Furthermore, neural activity is often scale-free, implying that some measurements should be the same, whether taken at large or small scales. Together, convergence and scale-freeness support the hypothesis that single V_m recordings carry useful information about high-dimensional cortical activity. Conveniently, the theory of "critical branching networks" (one purported explanation for scale-freeness) provides testable predictions about scale-free measurements that are readily applied to V_m fluctuations. To investigate, we obtained whole-cell current-clamp recordings of pyramidal neurons in visual cortex of turtles with unknown genders. We isolated fluctuations in V_m below the firing threshold and analyzed them by adapting the definition of "neuronal avalanches" (i.e., spurts of population spiking). The V_m fluctuations which we analyzed were scale-free and consistent with critical branching. These findings recapitulated results from large-scale cortical population data obtained separately in complementary experiments using microelectrode arrays described previously (Shew et al., 2015). Simultaneously recorded single-unit local field potential did not provide a good match, demonstrating the specific utility of V_m. Modeling shows that estimation of dynamical network properties from neuronal inputs is most accurate when networks are structured as critical branching networks. In conclusion, these findings extend evidence of critical phenomena while also establishing subthreshold pyramidal neuron V_m fluctuations as an informative gauge of high-dimensional cortical population activity.

SIGNIFICANCE STATEMENT The relationship between membrane potential (V_m) dynamics of single neurons and population dynamics is indispensable to understanding cortical circuits. Just as important to the biophysics of computation are emergent properties such as scale-freeness, where critical branching networks offer insight. This report makes progress on both fronts by comparing statistics from single-neuron whole-cell recordings with population statistics obtained with microelectrode arrays. Not only are fluctuations of somatic V_m scale-free, they match fluctuations of population activity. Thus, our results demonstrate appropriation of the brain's own subsampling method (convergence of synaptic inputs) while extending the range of fundamental evidence for critical phenomena in neural systems from the previously observed mesoscale (fMRI, LFP, population spiking) to the microscale, namely, V_m fluctuations.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Pedunculopontine Glutamatergic Neurons Provide a Novel Source of Feedforward Inhibition in the Striatum by Selectively Targeting Interneurons

The main excitatory inputs to the striatum arising from the cortex and the thalamus innervate both striatal spiny projection neurons and interneurons. These glutamatergic inputs to striatal GABAergic interneurons have been suggested to regulate the spike timing of striatal projection neurons via feedforward inhibition. Understanding how different excitatory inputs are integrated within the striatal circuitry and how they regulate striatal output is crucial for understanding basal ganglia function and related behaviors. Here, using VGLUT2 mice from both sexes, we report the existence of a glutamatergic projection from the mesencephalic locomotor region to the striatum that avoids the spiny neurons and selectively innervates interneurons. Specifically, optogenetic activation of glutamatergic axons from the pedunculopontine nucleus induced monosynaptic excitation in most recorded striatal cholinergic interneurons and GABAergic fast-spiking interneurons. Optogenetic stimulation in awake head-fixed mice consistently induced an increase in the firing rate of putative cholinergic interneurons and fast-spiking interneurons. In contrast, this stimulation did not induce excitatory responses in spiny neurons but rather disynaptic inhibitory responses ex vivo and a decrease in their firing rate in vivo, suggesting a feedforward mechanism mediating the inhibition of spiny projection neurons through the selective activation of striatal interneurons. Furthermore, unilateral stimulation of pedunculopontine nucleus glutamatergic axons in the striatum induced ipsilateral head rotations consistent with the inhibition of striatal output neurons. Our results demonstrate the existence of a unique interneuron-specific midbrain glutamatergic input to the striatum that exclusively recruits feedforward inhibition mechanisms.

SIGNIFICANCE STATEMENT Glutamatergic inputs to the striatum have been shown to target both striatal projection neurons and interneurons and have been proposed to regulate spike timing of the projection neurons in part through feedforward inhibition. Here, we reveal the existence of a midbrain source of glutamatergic innervation to the striatum, originating in the pedunculopontine nucleus. Remarkably, this novel input selectively targets striatal interneurons, avoiding the projection neurons. Furthermore, we show that this selective innervation of interneurons can regulate the firing of the spiny projection neurons and inhibit the striatal output via feedforward inhibition. Together, our results describe a unique source of excitatory innervation to the striatum which selectively recruits feedforward inhibition of spiny neurons without any accompanying excitation.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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The Spinal Transcriptome after Cortical Stroke: In Search of Molecular Factors Regulating Spontaneous Recovery in the Spinal Cord

In response to cortical stroke and unilateral corticospinal tract degeneration, compensatory sprouting of spared corticospinal fibers is associated with recovery of skilled movement in rodents. To date, little is known about the molecular mechanisms orchestrating this spontaneous rewiring. In this study, we provide insights into the molecular changes in the spinal cord tissue after large ischemic cortical injury in adult female mice, with a focus on factors that might influence the reinnervation process by contralesional corticospinal neurons. We mapped the area of cervical gray matter reinnervation by sprouting contralesional corticospinal axons after unilateral photothrombotic stroke of the motor cortex in mice using anterograde tracing. The mRNA profile of this reinnervation area was analyzed using whole-genome sequencing to identify differentially expressed genes at selected time points during the recovery process. Bioinformatic analysis revealed two phases of processes: early after stroke (4–7 d post-injury), the spinal transcriptome is characterized by inflammatory processes, including phagocytic processes as well as complement cascade activation. Microglia are specifically activated in the denervated corticospinal projection fields in this early phase. In a later phase (28–42 d post-injury), biological processes include tissue repair pathways with upregulated genes related to neurite outgrowth. Thus, the stroke-denervated spinal gray matter, in particular its intermediate laminae, represents a growth-promoting environment for sprouting corticospinal fibers originating from the contralesional motor cortex. This dataset provides a solid starting point for future studies addressing key elements of the post-stroke recovery process, with the goal to improve neuroregenerative treatment options for stroke patients.

SIGNIFICANCE STATEMENT We show that the molecular changes in the spinal cord target tissue of the stroke-affected corticospinal tract are mainly defined by two phases: an early inflammatory phase during which microglia are specifically activated in the target area of reinnervating corticospinal motor neurons; and a late phase during which growth-promoting factors are upregulated which can influence the sprouting response, arborization, and synapse formation. By defining for the first time the endogenous molecular machinery in the stroke-denervated cervical spinal gray matter with a focus on promotors of axon growth through the growth-inhibitory adult CNS, this study will serve as a basis to address novel neuroregenerative treatment options for chronic stroke patients.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Regeneration of Dopaminergic Neurons in Adult Zebrafish Depends on Immune System Activation and Differs for Distinct Populations

Adult zebrafish, in contrast to mammals, regenerate neurons in their brain, but the extent and variability of this capacity is unclear. Here we ask whether the loss of various dopaminergic neuron populations is sufficient to trigger their functional regeneration. Both sexes of zebrafish were analyzed. Genetic lineage tracing shows that specific diencephalic ependymo-radial glial (ERG) progenitor cells give rise to new dopaminergic [tyrosine hydroxylase-positive (TH⁺)] neurons. Ablation elicits an immune response, increased proliferation of ERG progenitor cells, and increased addition of new TH⁺ neurons in populations that constitutively add new neurons (e.g., diencephalic population 5/6). Inhibiting the immune response attenuates neurogenesis to control levels. Boosting the immune response enhances ERG proliferation, but not addition of TH⁺ neurons. In contrast, in populations in which constitutive neurogenesis is undetectable (e.g., the posterior tuberculum and locus ceruleus), cell replacement and tissue integration are incomplete and transient. This is associated with a loss of spinal TH⁺ axons, as well as permanent deficits in shoaling and reproductive behavior. Hence, dopaminergic neuron populations in the adult zebrafish brain show vast differences in regenerative capacity that correlate with constitutive addition of neurons and depend on immune system activation.

SIGNIFICANCE STATEMENT Despite the fact that zebrafish show a high propensity to regenerate neurons in the brain, this study reveals that not all types of dopaminergic neurons are functionally regenerated after specific ablation. Hence, in the same adult vertebrate brain, mechanisms of successful and incomplete regeneration can be studied. We identify progenitor cells for dopaminergic neurons and show that activating the immune system promotes the proliferation of these cells. However, in some areas of the brain this only leads to insufficient replacement of functionally important dopaminergic neurons that later disappear. Understanding the mechanisms of regeneration in zebrafish may inform interventions targeting the regeneration of functionally important neurons, such as dopaminergic neurons, from endogenous progenitor cells in nonregenerating mammals.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Reorganization of Recurrent Layer 5 Corticospinal Networks Following Adult Motor Training

Recurrent synaptic connections between neighboring neurons are a key feature of mammalian cortex, accounting for the vast majority of cortical inputs. Although computational models indicate that reorganization of recurrent connectivity is a primary driver of experience-dependent cortical tuning, the true biological features of recurrent network plasticity are not well identified. Indeed, whether rewiring of connections between cortical neurons occurs during behavioral training, as is widely predicted, remains unknown. Here, we probe M1 recurrent circuits following motor training in adult male rats and find robust synaptic reorganization among functionally related layer 5 neurons, resulting in a 2.5-fold increase in recurrent connection probability. This reorganization is specific to the neuronal subpopulation most relevant for executing the trained motor skill, and behavioral performance was impaired following targeted molecular inhibition of this subpopulation. In contrast, recurrent connectivity is unaffected among neighboring layer 5 neurons largely unrelated to the trained behavior. Training-related corticospinal cells also express increased excitability following training. These findings establish the presence of selective modifications in recurrent cortical networks in adulthood following training.

SIGNIFICANCE STATEMENT Recurrent synaptic connections between neighboring neurons are characteristic of cortical architecture, and modifications to these circuits are thought to underlie in part learning in the adult brain. We now show that there are robust changes in recurrent connections in the rat motor cortex upon training on a novel motor task. Motor training results in a 2.5-fold increase in recurrent connectivity, but only within the neuronal subpopulation most relevant for executing the new motor behavior; recurrent connectivity is unaffected among adjoining neurons that do not execute the trained behavior. These findings demonstrate selective reorganization of recurrent synaptic connections in the adult neocortex following novel motor experience, and illuminate fundamental properties of cortical function and plasticity.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Sexually Dimorphic Regulation of Behavioral States by Dopamine in Caenorhabditis elegans

Sex differences in behavior allow animals to effectively mate and reproduce. However, the mechanism by which biological sex regulates behavioral states, which underlie the regulation of sex-shared behaviors, such as locomotion, is largely unknown. In this study, we studied sex differences in the behavioral states of Caenorhabditis elegans and found that males spend less time in a low locomotor activity state than hermaphrodites and that dopamine generates this sex difference. In males, dopamine reduces the low activity state by acting in the same pathway as polycystic kidney disease-related genes that function in male-specific neurons. In hermaphrodites, dopamine increases the low activity state by suppression of octopamine signaling in the sex-shared SIA neurons, which have reduced responsiveness to octopamine in males. Furthermore, dopamine promotes exploration both inside and outside of bacterial lawn (the food source) in males and suppresses it in hermaphrodites. These results demonstrate that sexually dimorphic signaling allows the same neuromodulator to promote adaptive behavior for each sex.

SIGNIFICANCE STATEMENT The mechanisms that generate sex differences in sex-shared behaviors, including locomotion, are not well understood. We show that there are sex differences in the regulation of behavioral states in the model animal Caenorhabditis elegans. Dopamine promotes the high locomotor activity state in males, which must search for mates to reproduce, and suppresses it in self-fertilizing hermaphrodites through distinct molecular mechanisms. This study demonstrates that sex-specific signaling generates sex differences in the regulation of behavioral states, which in turn modulates the locomotor activity to suit reproduction for each sex.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Cell-Type-Specific Regulation of Nucleus Accumbens Synaptic Plasticity and Cocaine Reward Sensitivity by the Circadian Protein, NPAS2

The circadian transcription factor neuronal PAS domain 2 (NPAS2) is linked to psychiatric disorders associated with altered reward sensitivity. The expression of Npas2 is preferentially enriched in the mammalian forebrain, including the nucleus accumbens (NAc), a major neural substrate of motivated and reward behavior. Previously, we demonstrated that downregulation of NPAS2 in the NAc reduces the conditioned behavioral response to cocaine in mice. We also showed that Npas2 is preferentially enriched in dopamine receptor 1 containing medium spiny neurons (D1R-MSNs) of the striatum. To extend these studies, we investigated the impact of NPAS2 disruption on accumbal excitatory synaptic transmission and strength, along with the behavioral sensitivity to cocaine reward in a cell-type-specific manner. Viral-mediated knockdown of Npas2 in the NAc of male and female C57BL/6J mice increased the excitatory drive onto MSNs. Using Drd1a-tdTomato mice in combination with viral knockdown, we determined these synaptic adaptations were specific to D1R-MSNs relative to non-D1R-MSNs. Interestingly, NAc-specific knockdown of Npas2 blocked cocaine-induced enhancement of synaptic strength and glutamatergic transmission specifically onto D1R-MSNs. Last, we designed, validated, and used a novel Cre-inducible short-hairpin RNA virus for MSN-subtype-specific knockdown of Npas2. Cell-type-specific Npas2 knockdown in D1R-MSNs, but not D2R-MSNs, in the NAc reduced cocaine conditioned place preference. Together, our results demonstrate that NPAS2 regulates excitatory synapses of D1R-MSNs in the NAc and cocaine reward-related behavior.

SIGNIFICANCE STATEMENT Drug addiction is a widespread public health concern often comorbid with other psychiatric disorders. Disruptions of the circadian clock can predispose or exacerbate substance abuse in vulnerable individuals. We demonstrate a role for the core circadian protein, NPAS2, in mediating glutamatergic neurotransmission at medium spiny neurons (MSNs) in the nucleus accumbens (NAc), a region critical for reward processing. We find that NPAS2 negatively regulates functional excitatory synaptic plasticity in the NAc and is necessary for cocaine-induced plastic changes in MSNs expressing the dopamine 1 receptor (D1R). We further demonstrate disruption of NPAS2 in D1R-MSNs produces augmented cocaine preference. These findings highlight the significance of cell-type-specificity in mechanisms underlying reward regulation by NPAS2 and extend our knowledge of its function.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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PTCD1 Is Required for Mitochondrial Oxidative-Phosphorylation: Possible Genetic Association with Alzheimer's Disease

In addition to amyloid-β plaques and tau tangles, mitochondrial dysfunction is implicated in the pathology of Alzheimer's disease (AD). Neurons heavily rely on mitochondrial function, and deficits in brain energy metabolism are detected early in AD; however, direct human genetic evidence for mitochondrial involvement in AD pathogenesis is limited. We analyzed whole-exome sequencing data of 4549 AD cases and 3332 age-matched controls and discovered that rare protein altering variants in the gene pentatricopeptide repeat-containing protein 1 (PTCD1) show a trend for enrichment in cases compared with controls. We show here that PTCD1 is required for normal mitochondrial rRNA levels, proper assembly of the mitochondrial ribosome and hence for mitochondrial translation and assembly of the electron transport chain. Loss of PTCD1 function impairs oxidative phosphorylation and forces cells to rely on glycolysis for energy production. Cells expressing the AD-linked variant of PTCD1 fail to sustain energy production under increased metabolic stress. In neurons, reduced PTCD1 expression leads to lower ATP levels and impacts spontaneous synaptic activity. Thus, our study uncovers a possible link between a protein required for mitochondrial function and energy metabolism and AD risk.

SIGNIFICANCE STATEMENT Mitochondria are the main source of cellular energy and mitochondrial dysfunction is implicated in the pathology of Alzheimer's disease (AD) and other neurodegenerative disorders. Here, we identify a variant in the gene PTCD1 that is enriched in AD patients and demonstrate that PTCD1 is required for ATP generation through oxidative phosphorylation. PTCD1 regulates the level of 16S rRNA, the backbone of the mitoribosome, and is essential for mitochondrial translation and assembly of the electron transport chain. Cells expressing the AD-associated variant fail to maintain adequate ATP production during metabolic stress, and reduced PTCD1 activity disrupts neuronal energy homeostasis and dampens spontaneous transmission. Our work provides a mechanistic link between a protein required for mitochondrial function and genetic AD risk.

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Interferon-{gamma} as a Potential Link between Diabetes Mellitus and Dementia

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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This Week in The Journal

in Journal of Neuroscience current issue on June 12, 2019 04:30 PM.

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Dopamine Depletion Affects Vocal Acoustics and Disrupts Sensorimotor Adaptation in Songbirds

Dopamine is hypothesized to convey error information in reinforcement learning tasks with explicit appetitive or aversive cues. However, during motor skill learning feedback signals arise from an animal’s evaluation of sensory feedback resulting from its own behavior, rather than any external reward or punishment. It has previously been shown that intact dopaminergic signaling from the ventral tegmental area/substantia nigra pars compacta (VTA/SNc) complex is necessary for vocal learning when songbirds modify their vocalizations to avoid hearing distorted auditory feedback (playbacks of white noise). However, it remains unclear whether dopaminergic signaling underlies vocal learning in response to more naturalistic errors (pitch-shifted feedback delivered via headphones). We used male Bengalese finches (Lonchura striata var. domestica) to test the hypothesis that the necessity of dopamine signaling is shared between the two types of learning. We combined 6-hydroxydopamine (6-OHDA) lesions of dopaminergic terminals within Area X, a basal ganglia nucleus critical for song learning, with a headphones learning paradigm that shifted the pitch of auditory feedback and compared their learning to that of unlesioned controls. We found that 6-OHDA lesions affected song behavior in two ways. First, over a period of days lesioned birds systematically lowered their pitch regardless of the presence or absence of auditory errors. Second, 6-OHDA lesioned birds also displayed severe deficits in sensorimotor learning in response to pitch-shifted feedback. Our results suggest roles for dopamine in both motor production and auditory error processing, and a shared mechanism underlying vocal learning in response to both distorted and pitch-shifted auditory feedback.

in eNeuro current issue on June 12, 2019 04:30 PM.

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Lovastatin, not Simvastatin, Corrects Core Phenotypes in the Fragile X Mouse Model

The cholesterol-lowering drug lovastatin corrects neurological phenotypes in animal models of fragile X syndrome (FX), a commonly identified genetic cause of autism and intellectual disability (ID). The therapeutic efficacy of lovastatin is being tested in clinical trials for FX; however, the structurally similar drug simvastatin has been proposed as an alternative due to an increased potency and brain penetrance. Here, we perform a side-by-side comparison of the effects of lovastatin and simvastatin treatment on two core phenotypes in Fmr1^-/y mice versus WT littermates: excessive hippocampal protein synthesis and susceptibility to audiogenic seizures (AGSs). We find that simvastatin does not correct excessive hippocampal protein synthesis in the Fmr1^-/y hippocampus at any dose tested. In fact, simvastatin significantly increases protein synthesis in both Fmr1^-/y and WT. Moreover, injection of simvastatin does not reduce AGS in the Fmr1^-/y mouse, while lovastatin significantly reduces AGS incidence and severity versus vehicle-treated animals. These results show that unlike lovastatin, simvastatin does not correct core phenotypes in the Fmr1^-/y mouse model.

in eNeuro current issue on June 12, 2019 04:30 PM.

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The NeuroD6 Subtype of VTA Neurons Contributes to Psychostimulant Sensitization and Behavioral Reinforcement

Reward-related behavior is complex and its dysfunction correlated with neuropsychiatric illness. Dopamine (DA) neurons of the ventral tegmental area (VTA) have long been associated with different aspects of reward function, but it remains to be disentangled how distinct VTA DA neurons contribute to the full range of behaviors ascribed to the VTA. Here, a recently identified subtype of VTA neurons molecularly defined by NeuroD6 (NEX1M) was addressed. Among all VTA DA neurons, less than 15% were identified as positive for NeuroD6. In addition to dopaminergic markers, sparse NeuroD6 neurons expressed the vesicular glutamate transporter 2 (Vglut2) gene. To achieve manipulation of NeuroD6 VTA neurons, NeuroD6(NEX)-Cre-driven mouse genetics and optogenetics were implemented. First, expression of vesicular monoamine transporter 2 (VMAT2) was ablated to disrupt dopaminergic function in NeuroD6 VTA neurons. Comparing Vmat2^{lox/lox;NEX-Cre} conditional knock-out (cKO) mice with littermate controls, it was evident that baseline locomotion, preference for sugar and ethanol, and place preference upon amphetamine-induced and cocaine-induced conditioning were similar between genotypes. However, locomotion upon repeated psychostimulant administration was significantly elevated above control levels in cKO mice. Second, optogenetic activation of NEX-Cre VTA neurons was shown to induce DA release and glutamatergic postsynaptic currents within the nucleus accumbens. Third, optogenetic stimulation of NEX-Cre VTA neurons in vivo induced significant place preference behavior, while stimulation of VTA neurons defined by Calretinin failed to cause a similar response. The results show that NeuroD6 VTA neurons exert distinct regulation over specific aspects of reward-related behavior, findings that contribute to the current understanding of VTA neurocircuitry.

in eNeuro current issue on June 12, 2019 04:30 PM.

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Reciprocal Inhibitory Glomerular Circuits Contribute to Excitation-Inhibition Balance in the Mouse Olfactory Bulb

The major inhibitory interneurons in olfactory bulb (OB) glomeruli are periglomerular cells (PGCs) and short axon cells (SACs). PGCs and SACs provide feedforward inhibition to all classes of projection neurons, but inhibition between PGCs and SACs is not well understood. We crossed Cre and GFP transgenic mice and used virally-delivered optogenetic constructs to selectively activate either SACs or GAD65cre-ChR2-positive PGCs while recording from identified GAD65cre-ChR2-positive PGCs or SACs, respectively, to investigate inhibitory interactions between these two interneuron types. We show that GAD65cre-ChR2-positive PGCs robustly inhibit SACs and SACs strongly inhibit PGCs. SACs form the interglomerular circuit, which inhibits PGCs in distant glomeruli. Activation of GAD65cre-ChR2-positive PGCs monosynaptically inhibit mitral cells (MCs), which complements recent findings that SACs directly inhibit MCs. Thus, both classes of glomerular inhibitory neurons inhibit each other, as well as OB output neurons. We further show that olfactory nerve input to one glomerulus engages the interglomerular circuit and inhibits PGCs in distant glomeruli. Sensory activation of the interglomerular circuit directly inhibits output neurons in other glomeruli and by inhibiting intraglomerular PGCs, may potentially disinhibit output neurons in other glomeruli. The nature and context of odorant stimuli may determine whether inhibition or excitation prevails so that odors are represented in part by patterns of active and inactive glomeruli.

in eNeuro current issue on June 12, 2019 04:30 PM.

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Critical Analysis of Particle Detection Artifacts in Synaptosome Flow Cytometry

Flow cytometry and fluorescence-activated sorting are powerful techniques that hold great promise for studying heterogeneous populations of submicron particles such as synaptosomes, but many technical challenges arise in these experiments. To date, most flow cytometry studies of synaptosomes have relied on particle detection using forward scatter (FSC) measurements and size estimation with polystyrene (PS) bead standards. However, these practices have serious limitations, and special care must be taken to overcome the poor sensitivity of conventional flow cytometers in the analysis of submicron particles. Technical artifacts can confound these experiments, especially the detection of multiple particles as a single event. Here, we compared analysis of P2 crude synaptosomal preparations from murine forebrain on multiple flow cytometers using both FSC-triggered and fluorescence-triggered detection. We implemented multicolor fluorescent dye-based assays to quantify coincident particle detection and aggregation, and we assessed the false colocalization of antigens in immunostaining analyses. Our results demonstrate that fluorescence triggering and proper dilution can control for coincident particle detection, but not particle aggregation. We confirmed previous studies showing that FSC-based size estimation with PS beads underestimates biological particle size, and we identified pervasive aggregation in the FSC range analyzed in most synaptosome flow cytometry studies. We found that analyzing P2 samples in sucrose/EDTA/tris (SET) buffer reduces aggregation compared to PBS, but does not completely eliminate the presence of aggregates, especially in immunostaining experiments. Our study highlights challenges and pitfalls in synaptosome flow cytometry and provides a methodological framework for future studies.

in eNeuro current issue on June 12, 2019 04:30 PM.

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Corrigendum: Gap Junctions in A8 Amacrine Cells Are Made of Connexin36 but Are Differently Regulated Than Gap Junctions in AII Amacrine Cells

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Accelerated Age-Related Degradation of the Tectorial Membrane in the Ceacam16βgal/βgal Null Mutant Mouse, a Model for Late-Onset Human Hereditary Deafness DFNB113

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Elevated Serum SIRT 2 May Differentiate Parkinson’s Disease From Atypical Parkinsonian Syndromes

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Intracortical Inhibition and Surround Inhibition in the Motor Cortex: A TMS-EEG Study

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on June 12, 2019 12:00 AM.

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Canine Cognitive Dysfunction and Alzheimer’s Disease – Two Facets of the Same Disease?

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 12, 2019 12:00 AM.

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Classification of Multiple Sclerosis Clinical Profiles via Graph Convolutional Neural Networks

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 12, 2019 12:00 AM.

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Using the Wild Bootstrap to Quantify Uncertainty in Mean Apparent Propagator MRI

in Frontiers in Neuroinformatics | New and Recent Articles on June 12, 2019 12:00 AM.

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Disparities in Diffuse Cortical White Matter Integrity Between Socioeconomic Groups

in Frontiers in Human Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Corrigendum: The Binocular Balance at High Spatial Frequencies as Revealed by the Binocular Orientation Combination Task

in Frontiers in Human Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Neural Correlates of Verbal Working Memory: An fMRI Meta-Analysis

in Frontiers in Human Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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The Human Default Consciousness and Its Disruption: Insights From an EEG Study of Buddhist Jhāna Meditation

in Frontiers in Human Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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EEG Microstates Analysis in Young Adults With Autism Spectrum Disorder During Resting-State

in Frontiers in Human Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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DC Shifts-fMRI: A Supplement to Event-Related fMRI

in Frontiers in Computational Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Dynamic Factors for Transmitter Release at Small Presynaptic Boutons Revealed by Direct Patch-Clamp Recordings

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Acetylcholine Release Inhibits Distinct Excitatory Inputs Onto Hippocampal CA1 Pyramidal Neurons via Different Cellular and Network Mechanisms

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Hedgehog Pathway Activation Alters Ciliary Signaling in Primary Hypothalamic Cultures

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Synaptic FUS Localization During Motoneuron Development and Its Accumulation in Human ALS Synapses

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Co-transplantation of Epidermal Neural Crest Stem Cells and Olfactory Ensheathing Cells Repairs Sciatic Nerve Defects in Rats

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Activated PPARγ Abrogates Misprocessing of Amyloid Precursor Protein, Tau Missorting and Synaptotoxicity

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Mental Flexibility Influences the Association Between Poor Balance and Falls in Older People – A Secondary Analysis

in Frontiers in Aging Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Erratum: Cingulate Cortex Atrophy Is Associated With Hearing Loss in Presbycusis With Cochlear Amplifier Dysfunction

in Frontiers in Aging Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Insulin Resistance Is a Risk Factor for Overall Cerebral Small Vessel Disease Burden in Old Nondiabetic Healthy Adult Population

in Frontiers in Aging Neuroscience | New and Recent Articles on June 12, 2019 12:00 AM.

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Apamin Improves Prefrontal Nicotinic Impairment in Mouse Model of Alzheimer’s Disease

in Cerebral Cortex Advance Access on June 12, 2019 12:00 AM.

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A VTA GABAergic Neural Circuit Mediates Visually Evoked Innate Defensive Responses

in Neuron on June 12, 2019 12:00 AM.

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Prefrontal Cortex Regulates Sensory Filtering through a Basal Ganglia-to-Thalamus Pathway

in Neuron on June 12, 2019 12:00 AM.

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Parallel scalable simulations of biological neural networks using TensorFlow: A beginner's guide. (arXiv:1906.03958v1 [q-bio.NC])

Neuronal networks are often modeled as systems of coupled, nonlinear, ordinary or partial differential equations. The number of differential equations used to model a network increases with the size of the network and the level of detail used to model individual neurons and synapses. As one scales up the size of the simulation it becomes important to use powerful computing platforms. Many tools exist that solve these equations numerically. However, these tools are often platform specific. There is a high barrier of entry to developing flexible general purpose code that is platform independent and supports hardware acceleration on modern computing architectures such as GPUs/TPUs and Distributed Platforms. TensorFlow is a Python-based open-source package initially designed for machine learning algorithms, but it presents a scalable environment for a variety of computations including solving differential equations using iterative algorithms such as Runge Kutta methods. In this article, organized as a series of tutorials, we present a simple exposition of numerical methods to solve ordinary differential equations using Python and TensorFlow. It consists of a series of Python notebooks that, over the course of five sessions, will lead novice programmers from writing programs to integrate simple 1-dimensional differential equations using Python, to solving a large system (1000's of differential equations) of conductance-based neurons using a highly parallel and scalable framework. Embedded within the tutorial is a physiologically realistic implementation of a network in the insect olfactory system. This system, consisting of multiple neuron and synapse types, can serve as a template to simulate other networks.

in q-bio.NC updates on arXiv.org on June 11, 2019 01:30 AM.

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Secrets of the Brain: An Introduction to the Brain Anatomical Structure and Biological Function. (arXiv:1906.03314v1 [q-bio.NC])

In this paper, we will provide an introduction to the brain structure and function. Brain is an astonishing living organ inside our heads, weighing about 1.5kg, consisting of billions of tiny cells. The brain enables us to sense the world around us (to touch, to smell, to see and to hear, etc.), to think and to respond to the world as well. The main obstacles that prevent us from creating a machine which can behavior like real-world creatures are due to our limited knowledge about the brain in both its structure and its function. In this paper, we will focus introducing the brain anatomical structure and biological function, as well as its surrounding sensory systems. Many of the materials used in this paper are from wikipedia and several other neuroscience introductory articles, which will be properly cited in this article. This is the first of the three tutorial articles about the brain (the other two are [26] and [27]). In the follow-up two articles, we will further introduce the low-level composition basis structures (e.g., neuron, synapse and action potential) and the high-level cognitive functions (e.g., consciousness, attention, learning and memory) of the brain, respectively.

in q-bio.NC updates on arXiv.org on June 11, 2019 01:30 AM.

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Corrigendum: Patch-Seq Protocol to Analyze the Electrophysiology, Morphology and Transcriptome of Whole Single Neurons Derived From Human Pluripotent Stem Cells

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Effects of the LPA1 Receptor Deficiency and Stress on the Hippocampal LPA Species in Mice

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Neuroprotection by Therapeutic Hypothermia

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 11, 2019 12:00 AM.

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Spatial Resolution and Imaging Encoding fMRI Settings for Optimal Cortical and Subcortical Motor Somatotopy in the Human Brain

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 11, 2019 12:00 AM.

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Microstates as Disease and Progression Markers in Patients With Mild Cognitive Impairment

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 11, 2019 12:00 AM.

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Proteomics Approaches for Biomarker and Drug Target Discovery in ALS and FTD

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 11, 2019 12:00 AM.

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Modeling the Switching Behavior of Functional Connectivity Microstates (FCμstates) as a Novel Biomarker for Mild Cognitive Impairment

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 11, 2019 12:00 AM.

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Short Version Dental Anxiety Inventory Score May Predict the Response in the Insular Cortex to Stimuli Mimicking Dental Treatment

in Frontiers in Human Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Exploring the Neural Correlates in Adopting a Realistic View: A Neural Structural and Functional Connectivity Study With Female Nurses

in Frontiers in Human Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Motor Imagery of Speech: The Involvement of Primary Motor Cortex in Manual and Articulatory Motor Imagery

in Frontiers in Human Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Low Prefrontal GABA Levels Are Associated With Poor Cognitive Functions in Professional Boxers

in Frontiers in Human Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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EEG-Based Prediction of Cognitive Load in Intelligence Tests

in Frontiers in Human Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Touching! An Augmented Reality System for Unveiling Face Topography in Very Young Children

in Frontiers in Human Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Ability-Based Emotional Intelligence Is Associated With Greater Cardiac Vagal Control and Reactivity

in Frontiers in Human Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Inner Ear Therapeutics: An Overview of Middle Ear Delivery

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Alzheimer’s Disease Associated Genes Ankyrin and Tau Cause Shortened Lifespan and Memory Loss in Drosophila

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Merkel Cells Release Glutamate Following Mechanical Stimulation: Implication of Glutamate in the Merkel Cell-Neurite Complex

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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MEA6 Deficiency Impairs Cerebellar Development and Motor Performance by Tethering Protein Trafficking

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Sphingolipids as Emerging Mediators in Retina Degeneration

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Ketamine Within Clinically Effective Range Inhibits Glutamate Transmission From Astrocytes to Neurons and Disrupts Synchronization of Astrocytic SICs

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Commentary: The Nomenclature of Human White Matter Association Pathways: Proposal for a Systematic Taxonomic Anatomical Classification

in Frontiers in Neuroanatomy | New and Recent Articles on June 11, 2019 12:00 AM.

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Early-Onset Molecular Derangements in the Olfactory Bulb of Tg2576 Mice: Novel Insights Into the Stress-Responsive Olfactory Kinase Dynamics in Alzheimer’s Disease

in Frontiers in Aging Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Sleep, Aging, and Cellular Health: Aged-Related Changes in Sleep and Protein Homeostasis Converge in Neurodegenerative Diseases

in Frontiers in Aging Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Lifespan Changes in Network Structure and Network Topology Dynamics During Rest and Auditory Oddball Performance

in Frontiers in Aging Neuroscience | New and Recent Articles on June 11, 2019 12:00 AM.

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Evidence for Similar Prefrontal Structural and Functional Alterations in Male and Female Rats Following Chronic Stress or Glucocorticoid Exposure

in Cerebral Cortex Advance Access on June 11, 2019 12:00 AM.

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Cerebellar Contribution to Preparatory Activity in Motor Neocortex

in Neuron on June 11, 2019 12:00 AM.

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Open Source Brain: A Collaborative Resource for Visualizing, Analyzing, Simulating, and Developing Standardized Models of Neurons and Circuits

in Neuron on June 11, 2019 12:00 AM.

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Nociceptor deletion of Tsc2 enhances axon regeneration by inducing a conditioning injury response in dorsal root ganglia

Neurons of the peripheral nervous system are able to regenerate injured axons, a process requiring significant cellular resources to establish and maintain long-distance growth. Genetic activation of mTORC1, a potent regulator of cellular metabolism and protein translation, improves axon regeneration of peripheral neurons by an unresolved mechanism. To gain insight into this process, we activated mTORC1 signaling in mouse nociceptors via genetic deletion of its negative regulator Tsc2. Perinatal deletion of Tsc2 in nociceptors enhanced initial axon growth after sciatic nerve crush, however by three days post-injury axon elongation rate became similar to controls. mTORC1 inhibition prior to nerve injury was required to suppress the enhanced axon growth. Gene expression analysis in purified nociceptors revealed that Tsc2-deficient nociceptors had increased activity of regeneration-associated transcription factors (RATFs), including cJun and Atf3, in the absence of injury. Additionally, nociceptor deletion of Tsc2 activated satellite glial cells and macrophages in the dorsal root ganglia (DRG) in a similar manner to nerve injury. Surprisingly, these changes improved axon length but not percentage of initiating axons in dissociated cultures. The pro-regenerative environment in naïve DRG was recapitulated by AAV8-mediated deletion of Tsc2 in adult mice, suggesting that this phenotype does not result from a developmental effect. Consistently, AAV8-mediated Tsc2 deletion did not improve behavioral recovery after a sciatic nerve crush injury despite initially enhanced axon growth. Together, these data show that neuronal mTORC1 activation induces an incomplete pro-regenerative environment in the DRG that improves initial but not later axon growth after nerve injury.

Significance Statement Long distance axon regeneration poses a significant hurdle to recovery following nervous system injury. Increased mTORC1 signaling improves axon regeneration, however the underlying mechanisms are incompletely understood. We activated neuronal mTORC1 signaling by genetically deleting Tsc2 in Nav1.8-positive neurons perinatally or by AAV8-mediated viral infection in adult mice and observed improved short- but not long-term axon regeneration after sciatic nerve injury. We suggest that Tsc2 deletion promotes initial but not later peripheral axon regeneration by upregulating expression of neuronal pro-regenerative genes and activating non-neuronal responses in the surrounding environment. Activating mTORC1 signaling in peripheral neurons may provide therapeutic benefit in circumstances with poor initial growth such as after spinal cord injury to the dorsal column or peripheral nerve repair.

in RSS PAP on June 10, 2019 04:30 PM.

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Ryanodine Receptor 2 Contributes to Impaired Protein Localization in Cyclic Nucleotide-gated Channel Deficiency

The photoreceptor cyclic nucleotide-gated (CNG) channel plays a pivotal role in phototransduction and cellular calcium homeostasis. Mutations in the cone photoreceptor CNG channel subunits CNGA3 and CNGB3 are associated with achromatopsia and cone dystrophies. CNG channel deficiency leads to endoplasmic reticulum (ER) stress-associated cone apoptosis, protein mislocalization, and ER calcium dysregulation. This work investigated the potential mechanisms of protein mislocalization associated with ER calcium dysregulation using Cnga3-/- mice lacking ER Ca2+ channel ryanodine receptor 2 (RyR2) specifically in cones. Deletion of Ryr2 improved outer segment (OS) localization of the cone proteins M-opsin, S-opsin, and cone phosphodiesterase subunit α’ (PDE6C) and decreased inner segment localization. One-month-old Cnga3-/- mice showed approximately 30% of M-opsin, 55% of S-opsin, and 50% of PDE6C localized to the OS. Cnga3-/- mice with Ryr2 deletion at the same age showed almost 60% of M- opsin, 70% of S-opsin, and 70% of PDE6C localized to the OS. Deletion of Ryr2 nearly completely reversed elevations of the ER stress markers phospho-IRE1α and phospho-eIF2α and suppressed cone apoptosis. Consistent with the improved cone protein localization and reduced ER stress/cone apoptosis, cone survival was improved by deletion of Ryr2. The number of cones was increased by about 28% in 2-4 month-old Cnga3-/- mice with Ryr2 deletion, compared with age-matched Cnga3-/- mice. This work demonstrates a role of RyR2/ER calcium dysregulation in protein mislocalization, ER stress and cone death. The findings provide novel insights into the mechanisms of photoreceptor degeneration and support strategies targeting ER calcium regulation to manage retinal degeneration.

Significance Statement The cyclic nucleotide-gated (CNG) channel plays a pivotal role in phototransduction and photoreceptor calcium homeostasis. Mutations in the cone CNG channel subunits are associated with achromatopsia and cone dystrophies. CNG channel deficiency leads to endoplasmic reticulum (ER) stress-associated cone apoptosis, protein mislocalization, and ER calcium dysregulation. This work demonstrates a role of ER Ca2+ channel ryanodine receptor 2 and ER calcium dysregulation in protein mislocalization and subsequent ER stress and cone cell death. The findings provide novel insights into the mechanisms of photoreceptor degeneration. Altered calcium signaling and ER stress-associated cell death are common throughout retinal degenerative diseases. Thus, strategies targeting ER calcium regulation may help treat or slow photoreceptor degeneration.

in RSS PAP on June 10, 2019 04:30 PM.

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Vocal Motor Performance in Birdsong Requires Brain-Body Interaction

Significance statement Motor skill learning typically occurs in a period when the brain needs to navigate a body that is still growing and developing. How the changing body, neural circuit formation and motor coding influence each other remains unknown. Songbirds provide excellent model systems to study motor skill learning. It has recently been shown that songbird vocal muscles double in speed during sensorimotor learning. Here we argue that these contractile as well as morphological changes stem predominantly from use and only secondarily from hormones or genetic programs. This implies that muscle training constrains skill learning trajectories. As contractile muscle property changes must require altered motor codes for achieving the same acoustic targets, the final performance results from interactions between brain and body.

in RSS PAP on June 10, 2019 04:30 PM.

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Central nervous system regeneration is driven by microglia necroptosis and repopulation

Nature Neuroscience, Published online: 10 June 2019; doi:10.1038/s41593-019-0418-z

in Nature Neuroscience - Issue - nature.com science feeds on June 10, 2019 12:00 AM.

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Circuit mechanisms for the maintenance and manipulation of information in working memory

Nature Neuroscience, Published online: 10 June 2019; doi:10.1038/s41593-019-0414-3

in Nature Neuroscience - Issue - nature.com science feeds on June 10, 2019 12:00 AM.

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State-dependent decoupling of sensory and motor circuits underlies behavioral flexibility in Drosophila

Nature Neuroscience, Published online: 10 June 2019; doi:10.1038/s41593-019-0413-4

in Nature Neuroscience - Issue - nature.com science feeds on June 10, 2019 12:00 AM.

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Divergence in the functional organization of human and macaque auditory cortex revealed by fMRI responses to harmonic tones

Nature Neuroscience, Published online: 10 June 2019; doi:10.1038/s41593-019-0410-7

in Nature Neuroscience - Issue - nature.com science feeds on June 10, 2019 12:00 AM.

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Paraventricular Thalamus Projection Neurons Integrate Cortical and Hypothalamic Signals for Cue-Reward Processing

in Neuron on June 10, 2019 12:00 AM.

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Subcortical Substrates of Explore-Exploit Decisions in Primates

in Neuron on June 10, 2019 12:00 AM.

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Neuro-genetic plasticity of Caenorhabditis elegans behavioral thermal tolerance

in Most Recent Articles: BMC Neuroscience on June 10, 2019 12:00 AM.

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Contribution of FEF to attentional periodicity during visual search: a TMS study

Visual search, looking for a target embedded among distractors, has long been used to study attention. Current theories postulate a two-stage process in which early visual areas perform feature extraction, while higher-order regions perform attentional selection. Such a model implies iterative communication between low- and high-level regions to sequentially select candidate targets in the array, focus attention on these elements, and eventually permit target recognition. This leads to two independent predictions: (1) high-level, attentional regions and (2) early visual regions should both be involved periodically during the search. Here, we used Transcranial Magnetic Stimulation (TMS) applied over the Frontal-Eye Field (FEF) in humans, known to be involved in attentional selection, at various delays while observers performed a difficult, attentional search task. We observed a periodic pattern of interference at ~6 Hz (theta) suggesting that the FEF is periodically involved during this difficult search task. We further compared this result with two previous studies (Dugué et al., 2011; 2015a) in which a similar TMS procedure was applied over the early visual cortex (V1) while observers performed the same task. This analysis revealed the same pattern of interference, i.e. V1 is periodically involved during this difficult search task, at the theta frequency. Past V1 evidence reappraised for this paper, together with our current FEF results, confirm both of our independent predictions, and suggest that difficult search is supported by low- and high-level regions, each involved periodically at the theta frequency.

Significant statement Attention models postulate a two-stage process during visual search in which early visual regions perform feature extraction, while higher-order regions perform attentional selection, these two levels iteratively (periodically) communicating until target recognition. Using TMS, we tested whether there is a causal link between these brain regions and attentional search performance. Similar to past V1 evidence reappraised in this study, we showed that difficult attention search is supported in the FEF by periodic processing at the theta frequency (~6 Hz). Taken together, these two findings support the idea that difficult search tasks are processed by a hierarchical system involving low- and high-level regions, each involved periodically, and allowing successful attentional exploration. Nonetheless, their potential interactions remain to be demonstrated.

in RSS PAP on June 07, 2019 04:30 PM.

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Quantification of Phase-Amplitude Coupling in Neuronal Oscillations: Comparison of Phase-Locking Value, Mean Vector Length, Modulation Index, and Generalized-Linear-Modeling-Cross-Frequency-Coupling

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 07, 2019 12:00 AM.

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Diffusion MRI: Assessment of the Impact of Acquisition and Preprocessing Methods Using the BrainVISA-Diffuse Toolbox

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 07, 2019 12:00 AM.

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The Effects of NMDA Receptor Blockade on Sensory-Evoked Responses in Superficial Layers of the Rat Barrel Cortex

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 07, 2019 12:00 AM.

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Brain Aging and Electrophysiological Signaling: Revisiting the Spreading Depression Model

in Frontiers in Aging Neuroscience | New and Recent Articles on June 07, 2019 12:00 AM.

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Resting-State Functional Connectivity Is Associated With Cerebrospinal Fluid Levels of the Synaptic Protein NPTX2 in Non-demented Older Adults

in Frontiers in Aging Neuroscience | New and Recent Articles on June 07, 2019 12:00 AM.

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Precision Aging: Applying Precision Medicine to the Field of Cognitive Aging

in Frontiers in Aging Neuroscience | New and Recent Articles on June 07, 2019 12:00 AM.

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Corrigendum to: Histological and MRI Study of the Development of the Human Indusium Griseum

in Cerebral Cortex Advance Access on June 07, 2019 12:00 AM.

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Corrigendum to: Sensitive Period for Cognitive Repurposing of Human Visual Cortex

in Cerebral Cortex Advance Access on June 07, 2019 12:00 AM.

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Accelerating Structural Degeneration in Temporal Regions and Their Effects on Cognition in Aging of MCI Patients

in Cerebral Cortex Advance Access on June 07, 2019 12:00 AM.

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Pannexin 1 Regulates Network Ensembles and Dendritic Spine Development in Cortical Neurons

Dendritic spines are the postsynaptic targets of excitatory synaptic inputs that undergo extensive proliferation and maturation during the first postnatal month in mice. However, our understanding of the molecular mechanisms that regulate spines during this critical period is limited. Previous work has shown that pannexin 1 (Panx1) regulates neurite growth and synaptic plasticity. We therefore investigated the impact of global Panx1 KO on spontaneous cortical neuron activity using Ca²⁺ imaging and in silico network analysis. Panx1 KO increased both the number and size of spontaneous co-active cortical neuron network ensembles. To understand the basis for these findings, we investigated Panx1 expression in postnatal synaptosome preparations from early postnatal mouse cortex. Between 2 and 4 postnatal weeks, we observed a precipitous drop in cortical synaptosome protein levels of Panx1, suggesting it regulates synapse proliferation and/or maturation. At the same time points, we observed significant enrichment of the excitatory postsynaptic density proteins PSD-95, GluA1, and GluN2a in cortical synaptosomes from global Panx1 knock-out mice. Ex vivo analysis of pyramidal neuron structure in somatosensory cortex revealed a consistent increase in dendritic spine densities in both male and female Panx1 KO mice. Similar findings were observed in an excitatory neuron-specific Panx1 KO line (Emx1-Cre driven; Panx1 cKO^E) and in primary Panx1 KO cortical neurons cultured in vitro. Altogether, our study suggests that Panx1 negatively regulates cortical dendritic spine development.

in eNeuro current issue on June 06, 2019 04:31 PM.

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Handedness Matters for Motor Control But Not for Prediction

Skilled motor behavior relies on the ability to control the body and to predict the sensory consequences of this control. Although there is ample evidence that manual dexterity depends on handedness, it remains unclear whether control and prediction are similarly impacted. To address this issue, right-handed human participants performed two tasks with either the right or the left hand. In the first task, participants had to move a cursor with their hand so as to track a target that followed a quasi-random trajectory. This hand-tracking task allowed testing the ability to control the hand along an imposed trajectory. In the second task, participants had to track with their eyes a target that was self-moved through voluntary hand motion. This eye-tracking task allowed testing the ability to predict the visual consequences of hand movements. As expected, results showed that hand tracking was more accurate with the right hand than with the left hand. In contrast, eye tracking was similar in terms of spatial and temporal gaze attributes whether the target was moved by the right or the left hand. Although these results extend previous evidence for different levels of control by the two hands, they show that the ability to predict the visual consequences of self-generated actions does not depend on handedness. We propose that the greater dexterity exhibited by the dominant hand in many motor tasks stems from advantages in control, not in prediction. Finally, these findings support the notion that prediction and control are distinct processes.

in eNeuro current issue on June 06, 2019 04:31 PM.

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Reward Expectation Modulates Local Field Potentials, Spiking Activity and Spike-Field Coherence in the Primary Motor Cortex

Reward modulation of the primary motor cortex (M1) could be exploited in developing an autonomously updating brain-computer interface (BCI) based on a reinforcement learning (RL) architecture. For an autonomously updating RL based BCI system, we would need a reward prediction error, or a state-value representation from the user’s neural activity, which the RL-BCI agent could use to update its BCI-decoder. In order to understand the multifaceted effects of reward on M1 activity, we investigated how neural spiking, oscillatory activities and their functional interactions are modulated by conditioned stimuli related reward expectation. To do so, local field potentials (LFPs) and single-unit/multiunit activities were recorded simultaneously and bilaterally from M1 cortices while four non-human primates performed cued center-out reaching or grip force tasks either manually using their right arm/hand or observed passively. We found that reward expectation influenced the strength of alpha (8-14 Hz) power, alpha-gamma comodulation, alpha spike-field coherence, and firing rates in general in M1. Furthermore, we found that an increase in alpha-band power was correlated with a decrease in neural spiking activity, that firing rates were highest at the trough of the alpha-band cycle and lowest at the peak of its cycle. These findings imply that alpha oscillations modulated by reward expectation have an influence on spike firing rate and spike timing during both reaching and grasping tasks in M1. These LFP, spike, and spike-field interactions could be used to follow the M1 neural state in order to enhance BCI decoding (An et al., 2018; Zhao et al., 2018).

Significance Statement Knowing the subjective value of performed or observed actions is valuable feedback that could be used to improve the performance of an autonomously updating brain-computer interface (BCI). Reward-related information in the primary motor cortex (M1) may be crucial for more stable and robust BCI decoding (Zhao et al., 2018). Here, we present how expectation of reward during motor tasks, or simple observation, is represented by increased spike firing rates in conjunction with decreased alpha (8-14 Hz) oscillatory power, alpha-gamma comodulation, and alpha spike-field coherence, as compared to nonrewarding trials. Moreover, a phasic relation between alpha oscillations and firing rates was observed where firing rates were found to be lowest and highest at the peak and trough of alpha oscillations, respectively.

in RSS PAP on June 06, 2019 04:30 PM.

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Striatal circuits for reward learning and decision-making

Nature Reviews Neuroscience, Published online: 06 June 2019; doi:10.1038/s41583-019-0189-2

in Nature Reviews Neuroscience - Issue - nature.com science feeds on June 06, 2019 12:00 AM.

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Axon Guidance and Collective Cell Migration by Substrate-Derived Attractants

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 06, 2019 12:00 AM.

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Application of Graph Theory for Identifying Connectivity Patterns in Human Brain Networks: A Systematic Review

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on June 06, 2019 12:00 AM.

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Complex Electroresponsive Dynamics in Olivocerebellar Neurons Represented With Extended-Generalized Leaky Integrate and Fire Models

in Frontiers in Computational Neuroscience | New and Recent Articles on June 06, 2019 12:00 AM.

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Deletion of CD38 Suppresses Glial Activation and Neuroinflammation in a Mouse Model of Demyelination

in Frontiers in Cellular Neuroscience | New and Recent Articles on June 06, 2019 12:00 AM.

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Anatomical and Surgical Evaluation of the Common Marmoset as an Animal Model in Hearing Research

in Frontiers in Neuroanatomy | New and Recent Articles on June 06, 2019 12:00 AM.

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The Pre-synaptic Landscape of Mitral/Tufted Cells of the Main Olfactory Bulb

in Frontiers in Neuroanatomy | New and Recent Articles on June 06, 2019 12:00 AM.

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Phosphorylation and Dephosphorylation of Tau Protein During Synthetic Torpor

in Frontiers in Neuroanatomy | New and Recent Articles on June 06, 2019 12:00 AM.

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A Hyperkinetic Redox Sensor Drives Flies to Sleep

in Trends in Neurosciences on June 06, 2019 12:00 AM.

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Modulating Human Memory via Entrainment of Brain Oscillations

in Trends in Neurosciences on June 06, 2019 12:00 AM.

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Sleep Regulation by Neurotensinergic Neurons in a Thalamo-Amygdala Circuit

in Neuron on June 06, 2019 12:00 AM.

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Widespread and Highly Correlated Somato-dendritic Activity in Cortical Layer 5 Neurons

in Neuron on June 06, 2019 12:00 AM.

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The chromatin landscape of neuronal plasticity

Publication date: December 2019

Source: Current Opinion in Neurobiology, Volume 59

Author(s): Margaret Herre, Erica Korb

in ScienceDirect Publication: Current Opinion in Neurobiology on June 05, 2019 05:00 PM.

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TrkB-Shc Signaling Protects against Hippocampal Injury Following Status Epilepticus

Temporal lobe epilepsy (TLE) is a common and commonly devastating form of human epilepsy for which only symptomatic therapy is available. One cause of TLE is an episode of de novo prolonged seizures [status epilepticus (SE)]. Understanding the molecular signaling mechanisms by which SE transforms a brain from normal to epileptic may reveal novel targets for preventive and disease-modifying therapies. SE-induced activation of the BDNF receptor tyrosine kinase, TrkB, is one signaling pathway by which SE induces TLE. Although activation of TrkB signaling promotes development of epilepsy in this context, it also reduces SE-induced neuronal death. This led us to hypothesize that distinct signaling pathways downstream of TrkB mediate the desirable (neuroprotective) and undesirable (epileptogenesis) consequences. We subsequently demonstrated that TrkB-mediated activation of phospholipase C1 is required for epileptogenesis. Here we tested the hypothesis that the TrkB-Shc-Akt signaling pathway mediates the neuroprotective consequences of TrkB activation following SE. We studied measures of molecular signaling and cell death in a model of SE in mice of both sexes, including wild-type and TrkB^Shc/Shc mutant mice in which a point mutation (Y515F) of TrkB prevents the binding of Shc to activated TrkB kinase. Genetic disruption of TrkB-Shc signaling had no effect on severity of SE yet partially inhibited activation of the prosurvival adaptor protein Akt. Importantly, genetic disruption of TrkB-Shc signaling exacerbated hippocampal neuronal death induced by SE. We conclude that therapies targeting TrkB signaling for preventing epilepsy should spare TrkB-Shc-Akt signaling and thereby preserve the neuroprotective benefits.

SIGNIFICANCE STATEMENT Temporal lobe epilepsy (TLE) is a common and devastating form of human epilepsy that lacks preventive therapies. Understanding the molecular signaling mechanisms underlying the development of TLE may identify novel therapeutic targets. BDNF signaling thru TrkB receptor tyrosine kinase is one molecular mechanism promoting TLE. We previously discovered that TrkB-mediated activation of phospholipase C1 promotes epileptogenesis. Here we reveal that TrkB-mediated activation of Akt protects against hippocampal neuronal death in vivo following status epilepticus. These findings strengthen the evidence that desirable and undesirable consequences of status epilepticus-induced TrkB activation are mediated by distinct signaling pathways downstream of this receptor. These results provide a strong rationale for a novel therapeutic strategy selectively targeting individual signaling pathways downstream of TrkB for preventing epilepsy.

in Journal of Neuroscience current issue on June 05, 2019 04:30 PM.

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Astrocytic Epoxyeicosatrienoic Acid Signaling in the Medial Prefrontal Cortex Modulates Depressive-like Behaviors

Major depressive disorder is the most common mental illness. Mounting evidence indicates that astrocytes play a crucial role in the pathophysiology of depression; however, the underlying molecular mechanisms remain elusive. Compared with other neuronal cell types, astrocytes are enriched for arachidonic acid metabolism. Herein, we observed brain-region-specific alterations of epoxyeicosatrienoic acid (EET) signaling, which is an arachidonic acid metabolic pathway, in both a mouse model of depression and postmortem samples from patients with depression. The enzymatic activity of soluble epoxide hydrolase (sEH), the key enzyme in EET signaling, was selectively increased in the mPFC of susceptible mice after chronic social defeated stress and was negatively correlated with the social interaction ratio, which is an indicator of depressive-like behavior. The specific deletion of Ephx2 (encode sEH) in adult astrocytes induced resilience to stress, whereas the impaired EET signaling in the mPFC evoked depressive-like behaviors in response to stress. sEH was mainly expressed on lysosomes of astrocytes. Using pharmacological and genetic approaches performed on C57BL/6J background adult male mice, we found that EET signaling modulated astrocytic ATP release in vitro and in vivo. Moreover, astrocytic ATP release was required for the antidepressant-like effect of Ephx2 deletion in adult astrocytes. In addition, sEH inhibitors produced rapid antidepressant-like effects in multiple animal models of depression, including chronic social defeated stress and chronic mild stress. Together, our results highlight that EET signaling in astrocytes in the mPFC is essential for behavioral adaptation in response to psychiatric stress.

SIGNIFICANCE STATEMENT Astrocytes, the most abundant glial cells of the brain, play a vital role in the pathophysiology of depression. Astrocytes secrete adenosine ATP, which modulates depressive-like behaviors. Notably, astrocytes are enriched for arachidonic acid metabolism. In the present study, we explored the hypothesis that epoxyeicosatrienoic acid signaling, an arachidonic acid metabolic pathway, modulates astrocytic ATP release and the expression of depressive-like behaviors. Our work demonstrated that epoxyeicosatrienoic acid signaling in astrocytes in the mPFC is essential for behavioral homeostatic adaptation in response to stress, and the extent of astrocyte functioning is greater than expected based on earlier reports.

in Journal of Neuroscience current issue on June 05, 2019 04:30 PM.

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Reward-Related Expectations Trigger Dendritic Spine Plasticity in the Mouse Ventrolateral Orbitofrontal Cortex

An essential aspect of goal-directed decision-making is selecting actions based on anticipated consequences, a process that involves the orbitofrontal cortex (OFC) and potentially, the plasticity of dendritic spines in this region. To investigate this possibility, we trained male and female mice to nose poke for food reinforcers, or we delivered the same number of food reinforcers non-contingently to separate mice. We then decreased the likelihood of reinforcement for trained mice, requiring them to modify action–outcome expectations. In a separate experiment, we blocked action–outcome updating via chemogenetic inactivation of the OFC. In both cases, successfully selecting actions based on their likely consequences was associated with fewer immature, thin-shaped dendritic spines and a greater proportion of mature, mushroom-shaped spines in the ventrolateral OFC. This pattern was distinct from spine loss associated with aging, and we identified no effects on hippocampal CA1 neurons. Given that the OFC is involved in prospective calculations of likely outcomes, even when they are not observable, constraining spinogenesis while preserving mature spines may be important for solidifying durable expectations. To investigate causal relationships, we inhibited the RNA-binding protein fragile X mental retardation protein (encoded by Fmr1), which constrains dendritic spine turnover. Ventrolateral OFC-selective Fmr1 knockdown recapitulated the behavioral effects of inducible OFC inactivation (and lesions; also shown here), impairing action–outcome conditioning, and caused dendritic spine excess. Our findings suggest that a proper balance of dendritic spine plasticity within the OFC is necessary for one's ability to select actions based on anticipated consequences.

SIGNIFICANCE STATEMENT Navigating a changing environment requires associating actions with their likely outcomes and updating these associations when they change. Dendritic spine plasticity is likely involved, yet relationships are unconfirmed. Using behavioral, chemogenetic, and viral-mediated gene silencing strategies and high-resolution microscopy, we find that modifying action–outcome expectations is associated with fewer immature spines and a greater proportion of mature spines in the ventrolateral orbitofrontal cortex (OFC). Given that the OFC is involved in prospectively calculating the likely outcomes of one's behavior, even when they are not observable, constraining spinogenesis while preserving mature spines may be important for maintaining durable expectations.

in Journal of Neuroscience current issue on June 05, 2019 04:30 PM.

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Circuits That Mediate Expression of Signaled Active Avoidance Converge in the Pedunculopontine Tegmentum

An innocuous sensory stimulus that reliably signals an upcoming aversive event can be conditioned to elicit locomotion to a safe location before the aversive outcome ensues. The neural circuits that mediate the expression of this signaled locomotor action, known as signaled active avoidance, have not been identified. While exploring sensorimotor midbrain circuits in mice of either sex, we found that excitation of GABAergic cells in the substantia nigra pars reticulata blocks signaled active avoidance by inhibiting cells in the pedunculopontine tegmental nucleus (PPT), not by inhibiting cells in the superior colliculus or thalamus. Direct inhibition of putative-glutamatergic PPT cells, excitation of GABAergic PPT cells, or excitation of GABAergic afferents in PPT, abolish signaled active avoidance. Conversely, excitation of putative-glutamatergic PPT cells, or inhibition of GABAergic PPT cells, can be tuned to drive avoidance responses. The PPT is an essential junction for the expression of signaled active avoidance gated by nigral and other synaptic afferents.

SIGNIFICANCE STATEMENT When a harmful situation is signaled by a sensory stimulus (e.g., street light), subjects typically learn to respond with active or passive avoidance responses that circumvent the threat. During signaled active avoidance behavior, subjects move away to avoid a threat signaled by a preceding innocuous stimulus. We identified a part of the midbrain essential to process the signal and avoid the threat. Inhibition of neurons in this area eliminates avoidance responses to the signal but preserves escape responses caused by presentation of the threat. The results highlight an essential part of the neural circuits that mediate signaled active avoidance behavior.

in Journal of Neuroscience current issue on June 05, 2019 04:30 PM.

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Publisher Correction: Neuronal deletion of Gtf2i, associated with Williams syndrome, causes behavioral and myelin alterations rescuable by a remyelinating drug

Nature Neuroscience, Published online: 05 June 2019; doi:10.1038/s41593-019-0441-0

in Nature Neuroscience - Issue - nature.com science feeds on June 05, 2019 12:00 AM.

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Author Correction: GWAS of lifetime cannabis use reveals new risk loci, genetic overlap with psychiatric traits, and a causal effect of schizophrenia liability

Nature Neuroscience, Published online: 05 June 2019; doi:10.1038/s41593-019-0402-7

in Nature Neuroscience - Issue - nature.com science feeds on June 05, 2019 12:00 AM.

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Aberrant adaptive myelination in ‘chemobrain’

Nature Reviews Neuroscience, Published online: 05 June 2019; doi:10.1038/s41583-019-0194-5

in Nature Reviews Neuroscience - Issue - nature.com science feeds on June 05, 2019 12:00 AM.

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Hyperpolarization-Activated Cyclic Nucleotide-Gated Channels: An Emerging Role in Neurodegenerative Diseases

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 05, 2019 12:00 AM.

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Astrocyte, a Promising Target for Mood Disorder Interventions

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 05, 2019 12:00 AM.

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DMT1 Expression and Iron Levels at the Crossroads Between Aging and Neurodegeneration

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 05, 2019 12:00 AM.

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Increased Interleukin-6 Levels in the Astrocyte-Derived Exosomes of Sporadic Amyotrophic Lateral Sclerosis Patients

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 05, 2019 12:00 AM.

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Continuous Theta Burst Stimulation Over the Right Orbitofrontal Cortex Impairs Conscious Olfactory Perception

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on June 05, 2019 12:00 AM.

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Alcohol Dehydrogenase 1B Suppresses β-Amyloid-Induced Neuron Apoptosis

in Frontiers in Aging Neuroscience | New and Recent Articles on June 05, 2019 12:00 AM.

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Shaking Paws Is Not the Same as Shaking Hands

in Neuron on June 05, 2019 12:00 AM.

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Mitochondria Re-set Epilepsy

in Neuron on June 05, 2019 12:00 AM.

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A Chronic Pain in the ACC

in Neuron on June 05, 2019 12:00 AM.

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Leaving the Lights on Using Gamma Entrainment to Protect against Neurodegeneration

in Neuron on June 05, 2019 12:00 AM.

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Interneurons: Learning on the Job

in Neuron on June 05, 2019 12:00 AM.

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Central Amygdala Prepronociceptin-Expressing Neurons Mediate Palatable Food Consumption and Reward

in Neuron on June 05, 2019 12:00 AM.

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Publisher Correction: L3MBTL1 regulates ALS/FTD-associated proteotoxicity and quality control

Nature Neuroscience, Published online: 04 June 2019; doi:10.1038/s41593-019-0438-8

in Nature Neuroscience - Issue - nature.com science feeds on June 04, 2019 12:00 AM.

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Scn2a Haploinsufficiency in Mice Suppresses Hippocampal Neuronal Excitability, Excitatory Synaptic Drive, and Long-Term Potentiation, and Spatial Learning and Memory

in Frontiers in Molecular Neuroscience | New and Recent Articles on June 04, 2019 12:00 AM.

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Neurogenesis in Neurodegenerative Diseases: Role of MFG-E8

in Frontiers in Neuroscience | Neurogenesis section | New and Recent Articles on June 04, 2019 12:00 AM.

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Cortical Excitability Dynamics During Fear Processing

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on June 04, 2019 12:00 AM.

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Heterogeneous Nuclear Ribonucleoprotein E2 (hnRNP E2) Is a Component of TDP-43 Aggregates Specifically in the A and C Pathological Subtypes of Frontotemporal Lobar Degeneration

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 04, 2019 12:00 AM.

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Influence of Head Tissue Conductivity Uncertainties on EEG Dipole Reconstruction

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on June 04, 2019 12:00 AM.

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Role of the Blood-Brain Barrier in Central Nervous System Insulin Resistance

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on June 04, 2019 12:00 AM.

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Design and Development of Microscale Thickness Shear Mode (TSM) Resonators for Sensing Neuronal Adhesion

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on June 04, 2019 12:00 AM.

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Processing Pipeline for Atlas-Based Imaging Data Analysis of Structural and Functional Mouse Brain MRI (AIDAmri)

in Frontiers in Neuroinformatics | New and Recent Articles on June 04, 2019 12:00 AM.

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Exploiting Multi-Level Parallelism for Stitching Very Large Microscopy Images

in Frontiers in Neuroinformatics | New and Recent Articles on June 04, 2019 12:00 AM.

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Multi-Lag Analysis of Symbolic Entropies on EEG Recordings for Distress Recognition

in Frontiers in Neuroinformatics | New and Recent Articles on June 04, 2019 12:00 AM.

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Differences in Sodium Channel Densities in the Apical Dendrites of Pyramidal Cells of the Electrosensory Lateral Line Lobe

in Frontiers in Neural Circuits | New and Recent Articles on June 04, 2019 12:00 AM.

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Combined Assessment of Diffusion Parameters and Cerebral Blood Flow Within Basal Ganglia in Early Parkinson’s Disease

in Frontiers in Aging Neuroscience | New and Recent Articles on June 04, 2019 12:00 AM.

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Neurocompensatory Effects of the Default Network in Older Adults

in Frontiers in Aging Neuroscience | New and Recent Articles on June 04, 2019 12:00 AM.

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Brain–Heart Interactions Underlying Traditional Tibetan Buddhist Meditation

in Cerebral Cortex Advance Access on June 04, 2019 12:00 AM.

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Perineuronal Nets: Plasticity, Protection, and Therapeutic Potential

in Trends in Neurosciences on June 04, 2019 12:00 AM.

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Single-cell activity tracking reveals that orbitofrontal neurons acquire and maintain a long-term memory to guide behavioral adaptation

Nature Neuroscience, Published online: 03 June 2019; doi:10.1038/s41593-019-0408-1

in Nature Neuroscience - Issue - nature.com science feeds on June 03, 2019 12:00 AM.

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A supporting role

Nature Reviews Neuroscience, Published online: 03 June 2019; doi:10.1038/s41583-019-0193-6

in Nature Reviews Neuroscience - Issue - nature.com science feeds on June 03, 2019 12:00 AM.

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Reply to ‘Active and effective replay: systems consolidation reconsidered again’

Nature Reviews Neuroscience, Published online: 03 June 2019; doi:10.1038/s41583-019-0192-7

in Nature Reviews Neuroscience - Issue - nature.com science feeds on June 03, 2019 12:00 AM.

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Active and effective replay: systems consolidation reconsidered again

Nature Reviews Neuroscience, Published online: 03 June 2019; doi:10.1038/s41583-019-0191-8

in Nature Reviews Neuroscience - Issue - nature.com science feeds on June 03, 2019 12:00 AM.

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Editorial: The Superior Colliculus/Tectum: Cell Types, Circuits, Computations, Behaviors

in Frontiers in Neural Circuits | New and Recent Articles on June 03, 2019 12:00 AM.

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Endothelial Cells Filopodia in the Anastomosis of Central Nervous System Capillaries

in Frontiers in Neuroanatomy | New and Recent Articles on June 03, 2019 12:00 AM.

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Schizophrenia Exhibits Bi-directional Brain-Wide Alterations in Cortico-Striato-Cerebellar Circuits

in Cerebral Cortex Advance Access on June 03, 2019 12:00 AM.

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Studying Laboratory Mice – Into the Wild

in Trends in Neurosciences on June 03, 2019 12:00 AM.

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MeCP2: an epigenetic regulator of critical periods

Publication date: December 2019

Source: Current Opinion in Neurobiology, Volume 59

Author(s): Nathalie Picard, Michela Fagiolini

in ScienceDirect Publication: Current Opinion in Neurobiology on June 02, 2019 05:00 PM.

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The neuronal stimulation–transcription coupling map

Publication date: December 2019

Source: Current Opinion in Neurobiology, Volume 59

Author(s): Kelsey M Tyssowski, Jesse M Gray

in ScienceDirect Publication: Current Opinion in Neurobiology on June 02, 2019 05:00 PM.

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Glial regulation of synaptic function in models of addiction

Publication date: August 2019

Source: Current Opinion in Neurobiology, Volume 57

Author(s): David Stellwagen, Gina M Kemp, Simone Valade, Julien Chambon

in ScienceDirect Publication: Current Opinion in Neurobiology on June 02, 2019 05:00 PM.

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Subscription and Copyright Information

in Trends in Neurosciences on June 01, 2019 12:00 AM.

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Editorial Board and Contents

in Trends in Neurosciences on June 01, 2019 12:00 AM.

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Nanoscale Organization of Vesicle Release at Central Synapses

in Trends in Neurosciences on June 01, 2019 12:00 AM.

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SUMOylating Two Distinct Sites on the A-type Potassium Channel, Kv4.2, Increases Surface Expression and Decreases Current Amplitude

in Frontiers in Molecular Neuroscience | New and Recent Articles on May 31, 2019 12:00 AM.

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Elevated Levels of Arachidonic Acid-Derived Lipids Including Prostaglandins and Endocannabinoids Are Present Throughout ABHD12 Knockout Brains: Novel Insights Into the Neurodegenerative Phenotype

in Frontiers in Molecular Neuroscience | New and Recent Articles on May 31, 2019 12:00 AM.

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Novel Strategies for the Generation of Neuronal Diversity: Lessons From the Fly Visual System

in Frontiers in Molecular Neuroscience | New and Recent Articles on May 31, 2019 12:00 AM.

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Proestrus Differentially Regulates Expression of Ion Channel and Calcium Homeostasis Genes in GnRH Neurons of Mice

in Frontiers in Molecular Neuroscience | New and Recent Articles on May 31, 2019 12:00 AM.

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Resting-State Brain Network Dysfunctions Associated With Visuomotor Impairments in Autism Spectrum Disorder

in Frontiers in Integrative Neuroscience | New and Recent Articles on May 31, 2019 12:00 AM.

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Enhanced γ-Glutamyltranspeptidase Imaging That Unravels the Glioma Recurrence in Post-radio/Chemotherapy Mixtures for Precise Pathology via Enzyme-Triggered Fluorescent Probe

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on May 31, 2019 12:00 AM.

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A Crosstalk Between Brain Cholesterol Oxidation and Glucose Metabolism in Alzheimer’s Disease

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on May 31, 2019 12:00 AM.

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Inhomogeneities in Network Structure and Excitability Govern Initiation and Propagation of Spontaneous Burst Activity

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on May 31, 2019 12:00 AM.

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Diagnosis of Alzheimer’s Disease via Multi-Modality 3D Convolutional Neural Network

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on May 31, 2019 12:00 AM.

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Metabolic and Stress Response Changes Precede Disease Onset in the Spinal Cord of Mutant SOD1 ALS Mice

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on May 31, 2019 12:00 AM.

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Unsupervised Detection of Cell-Assembly Sequences by Similarity-Based Clustering

in Frontiers in Neuroinformatics | New and Recent Articles on May 31, 2019 12:00 AM.

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ELFENN: A Generalized Platform for Modeling Ephaptic Coupling in Spiking Neuron Models

in Frontiers in Neuroinformatics | New and Recent Articles on May 31, 2019 12:00 AM.

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Distribution of GABAergic Neurons and VGluT1 and VGAT Immunoreactive Boutons in the Ferret (Mustela putorius) Piriform Cortex and Endopiriform Nucleus. Comparison With Visual Areas 17, 18 and 19

in Frontiers in Neuroanatomy | New and Recent Articles on May 31, 2019 12:00 AM.

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The Anatomical Boundary of the Rat Claustrum

in Frontiers in Neuroanatomy | New and Recent Articles on May 31, 2019 12:00 AM.

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Lifespan Intellectual Factors, Genetic Susceptibility, and Cognitive Phenotypes in Aging: Implications for Interventions

in Frontiers in Aging Neuroscience | New and Recent Articles on May 31, 2019 12:00 AM.

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Working Memory Capacity as a Predictor of Cognitive Training Efficacy in the Elderly Population

in Frontiers in Aging Neuroscience | New and Recent Articles on May 31, 2019 12:00 AM.

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Addressing Disparities in Alzheimer's Disease and African-American Participation in Research: An Asset-Based Community Development Approach

in Frontiers in Aging Neuroscience | New and Recent Articles on May 31, 2019 12:00 AM.

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Humanin, a Mitochondrial-Derived Peptide Released by Astrocytes, Prevents Synapse Loss in Hippocampal Neurons

in Frontiers in Aging Neuroscience | New and Recent Articles on May 31, 2019 12:00 AM.

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New subtypes of allele-specific epigenetic effects: implications for brain development, function and disease

Publication date: December 2019

Source: Current Opinion in Neurobiology, Volume 59

Author(s): Stephanie N Kravitz, Christopher Gregg

in ScienceDirect Publication: Current Opinion in Neurobiology on May 30, 2019 05:00 PM.

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Adaptive learning under expected and unexpected uncertainty

Nature Reviews Neuroscience, Published online: 30 May 2019; doi:10.1038/s41583-019-0180-y

in Nature Reviews Neuroscience - Issue - nature.com science feeds on May 30, 2019 12:00 AM.

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Monoamine Oxidases (MAOs) as Privileged Molecular Targets in Neuroscience: Research Literature Analysis

in Frontiers in Molecular Neuroscience | New and Recent Articles on May 29, 2019 12:00 AM.

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Editorial: Bayesian Estimation and Inference in Computational Anatomy and Neuroimaging: Methods and Applications

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on May 29, 2019 12:00 AM.

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Linking the Endoplasmic Reticulum to Parkinson’s Disease and Alpha-Synucleinopathy

in Frontiers in Neuroscience | Neurodegeneration section | New and Recent Articles on May 29, 2019 12:00 AM.

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Impact of Sleep–Wake-Associated Neuromodulators and Repetitive Low-Frequency Stimulation on Human iPSC-Derived Neurons

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on May 29, 2019 12:00 AM.

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Antiepileptic Effects of a Novel Non-invasive Neuromodulation Treatment in a Subject With Early-Onset Epileptic Encephalopathy: Case Report With 20 Sessions of HD-tDCS Intervention

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on May 29, 2019 12:00 AM.

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How Do Price and Quantity Promotions Affect Hedonic Purchases? An ERPs Study

in Frontiers in Neuroscience | Neural Technology section | New and Recent Articles on May 29, 2019 12:00 AM.

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Editorial: Collaborative Efforts for Understanding the Human Brain

in Frontiers in Neuroinformatics | New and Recent Articles on May 29, 2019 12:00 AM.

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Evaluation of Enhanced Learning Techniques for Segmenting Ischaemic Stroke Lesions in Brain Magnetic Resonance Perfusion Images Using a Convolutional Neural Network Scheme

in Frontiers in Neuroinformatics | New and Recent Articles on May 29, 2019 12:00 AM.

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Editorial: The Functional Anatomy of the Reticular Formation

in Frontiers in Neuroanatomy | New and Recent Articles on May 29, 2019 12:00 AM.

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Iron concentrations in neurons and glial cells with estimates on ferritin concentrations

in Most Recent Articles: BMC Neuroscience on May 29, 2019 12:00 AM.

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Regulation of neuronal connectivity in the mammalian brain by chromatin remodeling

Publication date: December 2019

Source: Current Opinion in Neurobiology, Volume 59

Author(s): Jared V. Goodman, Azad Bonni

in ScienceDirect Publication: Current Opinion in Neurobiology on May 28, 2019 11:00 AM.

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Relaying ageing signals

Nature Reviews Neuroscience, Published online: 28 May 2019; doi:10.1038/s41583-019-0190-9

in Nature Reviews Neuroscience - Issue - nature.com science feeds on May 28, 2019 12:00 AM.

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Comparing integration and contextual binding accounts of memory impairment

Nature Reviews Neuroscience, Published online: 28 May 2019; doi:10.1038/s41583-019-0188-3

in Nature Reviews Neuroscience - Issue - nature.com science feeds on May 28, 2019 12:00 AM.

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Using second-person neuroscience to elucidate the mechanisms of social interaction

Nature Reviews Neuroscience, Published online: 28 May 2019; doi:10.1038/s41583-019-0179-4

in Nature Reviews Neuroscience - Issue - nature.com science feeds on May 28, 2019 12:00 AM.

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Unsupervised Temporal Contiguity Experience Does Not Break the Invariance of Orientation Selectivity Across Spatial Frequency

in Frontiers in Systems Neuroscience | New and Recent Articles on May 28, 2019 12:00 AM.

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Lysophosphatidic Acid and Glutamatergic Transmission

in Frontiers in Molecular Neuroscience | New and Recent Articles on May 28, 2019 12:00 AM.

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Structural and Functional Abnormalities in the Olfactory System of Fragile X Syndrome Models

in Frontiers in Molecular Neuroscience | New and Recent Articles on May 28, 2019 12:00 AM.

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Resilience and Vulnerability to Trauma: Early Life Interventions Modulate Aversive Memory Reconsolidation in the Dorsal Hippocampus

in Frontiers in Molecular Neuroscience | New and Recent Articles on May 28, 2019 12:00 AM.

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Neuronal Cells Rearrangement During Aging and Neurodegenerative Disease: Metabolism, Oxidative Stress and Organelles Dynamic

in Frontiers in Molecular Neuroscience | New and Recent Articles on May 28, 2019 12:00 AM.

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Characterizing the Structural Pattern Predicting Medication Response in Herpes Zoster Patients Using Multivoxel Pattern Analysis

in Frontiers in Neuroscience | Brain Imaging Methods section | New and Recent Articles on May 28, 2019 12:00 AM.