Discovery and Validation of Novel Genes in a Large Chinese Autism Spectrum Disorder Cohort

自闭症谱系障碍 候选基因 遗传学 自闭症 外显子组测序 基因 神经发育障碍 生物 智力残疾 拷贝数变化 人类遗传学 外显子组 遗传建筑学 人口 基因组 心理学 医学 突变 发展心理学 表型 环境卫生
作者
Li Wang,Juehua Yu,Mengdi Wang,Lingli Zhang,Kan Yang,Xiujuan Du,Jinyu Wu,Xiaoqun Wang,Fĕi Li,Zilong Qiu
出处
期刊:Biological Psychiatry [Elsevier]
卷期号:94 (10): 792-803 被引量:8
标识
DOI:10.1016/j.biopsych.2023.06.025
摘要

Autism spectrum disorder (ASD) is a neurodevelopmental disorder that causes impairments in social communication and stereotypical behaviors, often accompanied by developmental delay or intellectual disability. A growing body of evidence suggests that ASD is highly heritable, and genetic studies have defined numerous risk genes. However, most studies have been conducted with individuals of European and Hispanic ancestry, and there is a lack of genetic analyses of ASD in the East Asian population.We performed whole-exome sequencing on 772 Chinese ASD trios and combined the data with a previous study of 369 Chinese ASD trios, identifying de novo variants in 1141 ASD trios. We used single-cell RNA sequencing analysis to identify the cell types in which ASD-related genes were enriched. In addition, we validated the function of a candidate high-functioning autism gene in mouse models using genetic approaches.Our findings showed that ASD without developmental delay or intellectual disability carried fewer disruptive de novo variants than ASD with developmental delay or intellectual disability. Moreover, we identified 9 novel ASD candidate genes that were not present in the current ASD gene database. We further validated one such novel ASD candidate gene, SLC35G1, by showing that mice harboring a heterozygous deletion of Slc35g1 exhibited defects in interactive social behaviors.Our work nominates novel ASD candidate genes and emphasizes the importance of genome-wide genetic studies with ASD cohorts of different ancestries to reveal the comprehensive genetic architecture of ASD.
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