Gabrb3 is required for the functional integration of pyramidal neuron subtypes in the somatosensory cortex

Gabrb3 是体感皮层中锥体神经元亚型功能整合所必需的

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作者:Rachel Babij, Camilo Ferrer, Alexander Donatelle, Sam Wacks, Amanda M Buch, James E Niemeyer, Hongtao Ma, Zhe Ran S Duan, Robert N Fetcho, Alicia Che, Takumi Otsuka, Theodore H Schwartz, Ben S Huang, Conor Liston, Natalia V De Marco García

Abstract

Dysfunction of gamma-aminobutyric acid (GABA)ergic circuits is strongly associated with neurodevelopmental disorders. However, it is unclear how genetic predispositions impact circuit assembly. Using in vivo two-photon and widefield calcium imaging in developing mice, we show that Gabrb3, a gene strongly associated with autism spectrum disorder (ASD) and Angelman syndrome (AS), is enriched in contralaterally projecting pyramidal neurons and is required for inhibitory function. We report that Gabrb3 ablation leads to a developmental decrease in GABAergic synapses, increased local network synchrony, and long-lasting enhancement in functional connectivity of contralateral-but not ipsilateral-pyramidal neuron subtypes. In addition, Gabrb3 deletion leads to increased cortical response to tactile stimulation at neonatal stages. Using human transcriptomics and neuroimaging datasets from ASD subjects, we show that the spatial distribution of GABRB3 expression correlates with atypical connectivity in these subjects. Our studies reveal a requirement for Gabrb3 during the emergence of interhemispheric circuits for sensory processing.

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