Variance and invariance of neuronal long-term representations

Clopath, Claudia; Bonhoeffer, Tobias; Hübener, Mark; Rose, Tobias

doi:10.1098/rstb.2016.0161

Cited by 133 publications

(175 citation statements)

References 102 publications

(309 reference statements)

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“…the fraction of cells that were active at the given imaging time point and remained active in each of the following imaging sessions. In WT mice, the reoccurrence rates of active cells steadily declined throughout the imaging period, consistent with previous studies describing a high variability of neuronal activity patterns in the motor cortex (Rokni et al, 2007;Peters et al, 2014;Clopath et al, 2017). In R6/2 animals this decline also occurred, but slowed down from 8.5 weeks onwards, resulting in a higher reoccurrence rate compared to WT controls (WT, 7 FOVs from 6 mice; R6/2, 10 FOVs from 5 mice; Repeated measures ANOVA, 6.5 to 9.5 weeks:…”

Section: Altered Dynamics Of Single-cell Activity In Hd Micesupporting

confidence: 90%

Cortical circuit alterations precede disease onset in Huntington’s disease mice

Neuner

Schulz-Trieglaff

Gutiérrez-Ángel

et al. 2018

Preprint

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Huntington’s disease (HD) is a devastating hereditary movement disorder, characterized by degeneration of neurons in the striatum and cortex. Studies in human patients and mouse HD models suggest that disturbances of neuronal function in the neocortex play an important role in the disease onset and progression. However, the precise nature and time course of cortical alterations in HD have remained elusive. Here, we use chronic in vivo two-photon calcium imaging to monitor the activity of single neurons in layer 2/3 of the primary motor cortex in awake, behaving R6/2 transgenic HD mice and wildtype littermates. R6/2 mice show age-dependent changes in neuronal activity with a clear increase in activity at the age of 8.5 weeks, preceding the onset of motor and neurological symptoms. Furthermore, quantitative proteomics demonstrate a pronounced downregulation of synaptic proteins in the cortex, and histological analyses in R6/2 mice and HD patient samples reveal reduced inputs from parvalbumin-positive interneurons onto layer 2/3 pyramidal cells. Thus, our study provides a time-resolved description as well as mechanistic details of cortical circuit dysfunction in HD.Significance statementFuntional alterations in the cortex are believed to play an important role in the pathogenesis of Huntington’s disease (HD). However, studies monitoring cortical activity in HD models in vivo at a single-cell resultion are still lacking. We have used chronic two-photon imaging to investigate changes in the activity of single neurons in the primary motor cortex of awake presymptomatic HD mice. We show that neuronal activity increases before the mice develop disease symptoms. Our histological analyses in mice and in human HD autopsy cases furthermore demonstrate a loss inhibitory synaptic terminals from parvalbimun-positive interneurons, revealing a potential mechanism of cortical circuit impairment in HD.

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Section: Altered Dynamics Of Single-cell Activity In Hd Micesupporting

confidence: 90%

Cortical circuit alterations precede disease onset in Huntington’s disease mice

Neuner

Schulz-Trieglaff

Gutiérrez-Ángel

et al. 2018

Preprint

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“…Similarly, mechanisms involved in the recovery of individual neurons tuning following sensory deprivation in vivo [11,12,[14][15][16]29,60,67,95] could be explained via theoretical work. Theoretical models using attractor dynamics or hidden states [96,97] could be implemented to better understand how interactions between individual cells and the network of cells facilitate the recovery of activity following deprivation and maintain the same properties of individual cells from prior to deprivation [95,98]. Overall, better interaction between molecular/cellular and systems level experiments and theory will be critical to understand the underlying details of the mechanisms of plasticity and how they are implemented in vivo.…”

Section: Similarities Across Brain Regions In Vivomentioning

confidence: 99%

Integrating Hebbian and homeostatic plasticity: the current state of the field and future research directions

Keck

Toyoizumi

Chen

et al. 2017

Phil. Trans. R. Soc. B

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194

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We summarize here the results presented and subsequent discussion from the meeting on Integrating Hebbian and Homeostatic Plasticity at the Royal Society in April 2016. We first outline the major themes and results presented at the meeting. We next provide a synopsis of the outstanding questions that emerged from the discussion at the end of the meeting and finally suggest potential directions of research that we believe are most promising to develop an understanding of how these two forms of plasticity interact to facilitate functional changes in the brain.This article is part of the themed issue 'Integrating Hebbian and homeostatic plasticity'.

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“…Advances in neural imaging techniques allow us to interrogate such changes by tracking stimulus responses of hundreds of neurons over many days in vivo (Andermann, 2010;Mank et al, 2008). These recordings reveal a substantial, and puzzling, variability in the long-term stability of responses in sensory cortex: some neurons retain highly stable preferences to specific stimuli, whereas the stimulus preference of other neurons change from day to day (Ranson, 2017;Clopath and Rose, 2017;Rose et al, 2016;Poort et al, 2015;Lütcke et al, 2013). The degree of stimulus response stability typically depends on brain region; whisking responses in mouse barrel cortex are highly plastic, whereas visual responses in mouse V1 are more stable but still exhibit fluctuations (Clopath and Rose, 2017;Lütcke et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

Population coupling predicts the plasticity of stimulus responses in cortical circuits

Sweeney

Clopath

2018

Preprint

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Long-term imaging of sensory cortex reveals a diverse range of stimulus response stability: some neurons retain stimulus responses that are stable over days whereas other neurons have highly plastic stimulus responses. Using a recurrent network model, we explore whether this observation could be due to an underlying diversity in the synaptic plasticity of neurons. We find that, in a network with diverse learning rates, neurons with fast rates are more coupled to population activity than neurons with slow rates. This phenomenon, which we call a plasticity-coupling link, surprisingly predicts that neurons with high population coupling exhibit more long-term stimulus response variability than neurons with low population coupling. We substantiate this prediction using recordings from the Allen Brain Observatory which track the orientation preferences of 15,000 neurons in mouse visual cortex.In agreement with our model, a neuron's population coupling is correlated with the plasticity of its orientation preference. Finally, we show that high population coupling helps plastic neurons alter their stimulus preference during perceptual learning, but hinders the ability of stable neurons to provide an instructive signal for learning. This suggests a particular functional architecture: a stable 'backbone' of stimulus representation formed by neurons with slow synaptic plasticity and low population coupling, on top of which lies a flexible substrate of neurons with fast synaptic plasticity and high population coupling.

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Variance and invariance of neuronal long-term representations

Cited by 133 publications

References 102 publications

Cortical circuit alterations precede disease onset in Huntington’s disease mice

Cortical circuit alterations precede disease onset in Huntington’s disease mice

Integrating Hebbian and homeostatic plasticity: the current state of the field and future research directions

Population coupling predicts the plasticity of stimulus responses in cortical circuits

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