Distinct subnetworks of the thalamic reticular nucleus

被引:0
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作者
Yinqing Li
Violeta G. Lopez-Huerta
Xian Adiconis
Kirsten Levandowski
Soonwook Choi
Sean K. Simmons
Mario A. Arias-Garcia
Baolin Guo
Annie Y. Yao
Timothy R. Blosser
Ralf D. Wimmer
Tomomi Aida
Alexander Atamian
Tina Naik
Xuyun Sun
Dasheng Bi
Diya Malhotra
Cynthia C. Hession
Reut Shema
Marcos Gomes
Taibo Li
Eunjin Hwang
Alexandra Krol
Monika Kowalczyk
João Peça
Gang Pan
Michael M. Halassa
Joshua Z. Levin
Zhanyan Fu
Guoping Feng
机构
[1] Tsinghua University,School of Pharmaceutical Sciences, IDG/McGovern Institute for Brain Research, Center for Synthetic and Systems Biology
[2] Broad Institute of MIT and Harvard,The Stanley Center for Psychiatric Research
[3] Massachusetts Institute of Technology,McGovern Institute for Brain Research and the Department of Brain and Cognitive Sciences
[4] National Autonomous University of Mexico,Institute of Cellular Physiology
[5] Broad Institute of MIT and Harvard,Klarman Cell Observatory
[6] National Autonomous University of Mexico,Faculty of Psychology
[7] Zhejiang University,College of Computer Science and Technology
[8] Center for Neuroscience and Cell Biology,University of Coimbra
[9] University of Coimbra,Center for Neuroscience
[10] Institute for Interdisciplinary Research,undefined
[11] Korea Institute of Science and Technology,undefined
[12] University of Coimbra,undefined
[13] Department of Life Sciences,undefined
来源
Nature | 2020年 / 583卷
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摘要
The thalamic reticular nucleus (TRN), the major source of thalamic inhibition, regulates thalamocortical interactions that are critical for sensory processing, attention and cognition1–5. TRN dysfunction has been linked to sensory abnormality, attention deficit and sleep disturbance across multiple neurodevelopmental disorders6–9. However, little is known about the organizational principles that underlie its divergent functions. Here we performed an integrative study linking single-cell molecular and electrophysiological features of the mouse TRN to connectivity and systems-level function. We found that cellular heterogeneity in the TRN is characterized by a transcriptomic gradient of two negatively correlated gene-expression profiles, each containing hundreds of genes. Neurons in the extremes of this transcriptomic gradient express mutually exclusive markers, exhibit core or shell-like anatomical structure and have distinct electrophysiological properties. The two TRN subpopulations make differential connections with the functionally distinct first-order and higher-order thalamic nuclei to form molecularly defined TRN–thalamus subnetworks. Selective perturbation of the two subnetworks in vivo revealed their differential role in regulating sleep. In sum, our study provides a comprehensive atlas of TRN neurons at single-cell resolution and links molecularly defined subnetworks to the functional organization of thalamocortical circuits.
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页码:819 / 824
页数:5
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