Distinct subnetworks of the thalamic reticular nucleus

丘脑网状核的不同子网络

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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

Abstract

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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