| Literature DB >> 34197733 |
Dheeraj S Roy1, Ying Zhang2, Tomomi Aida2, Soonwook Choi3, Qian Chen2, Yuanyuan Hou2, Nicholas E Lea2, Keith M Skaggs2, Juliana C Quay2, Min Liew2, Hannah Maisano2, Vinh Le2, Carter Jones3, Jie Xu4, Dong Kong4, Heather A Sullivan2, Arpiar Saunders5, Steven A McCarroll5, Ian R Wickersham2, Guoping Feng6.
Abstract
Neuropsychiatric disorders are often accompanied by cognitive impairments/intellectual disability (ID). It is not clear whether there are converging mechanisms underlying these debilitating impairments. We found that many autism and schizophrenia risk genes are expressed in the anterodorsal subdivision (AD) of anterior thalamic nuclei, which has reciprocal connectivity with learning and memory structures. CRISPR-Cas9 knockdown of multiple risk genes selectively in AD thalamus led to memory deficits. While the AD is necessary for contextual memory encoding, the neighboring anteroventral subdivision (AV) regulates memory specificity. These distinct functions of AD and AV are mediated through their projections to retrosplenial cortex, using differential mechanisms. Furthermore, knockdown of autism and schizophrenia risk genes PTCHD1, YWHAG, or HERC1 from AD led to neuronal hyperexcitability, and normalization of hyperexcitability rescued memory deficits in these models. This study identifies converging cellular to circuit mechanisms underlying cognitive deficits in a subset of neuropsychiatric disease models.Entities:
Keywords: anterior thalamic nuclei; autism; cognition; memory; neuropsychiatric disorders; retrosplenial; schizophrenia; thalamus
Mesh:
Year: 2021 PMID: 34197733 PMCID: PMC8376805 DOI: 10.1016/j.neuron.2021.06.005
Source DB: PubMed Journal: Neuron ISSN: 0896-6273 Impact factor: 18.688