| Literature DB >> 32732423 |
Siwei Zhang1, Hanwen Zhang1, Yifan Zhou2,3, Min Qiao2,4, Siming Zhao2, Alena Kozlova1, Jianxin Shi5, Alan R Sanders1,6, Gao Wang2, Kaixuan Luo2, Subhajit Sengupta1, Siobhan West1, Sheng Qian2, Michael Streit1, Dimitrios Avramopoulos7, Chad A Cowan8, Mengjie Chen9, Zhiping P Pang10, Pablo V Gejman1,6, Xin He11,12, Jubao Duan13,6.
Abstract
Most neuropsychiatric disease risk variants are in noncoding sequences and lack functional interpretation. Because regulatory sequences often reside in open chromatin, we reasoned that neuropsychiatric disease risk variants may affect chromatin accessibility during neurodevelopment. Using human induced pluripotent stem cell (iPSC)-derived neurons that model developing brains, we identified thousands of genetic variants exhibiting allele-specific open chromatin (ASoC). These neuronal ASoCs were partially driven by altered transcription factor binding, overrepresented in brain gene enhancers and expression quantitative trait loci, and frequently associated with distal genes through chromatin contacts. ASoCs were enriched for genetic variants associated with brain disorders, enabling identification of functional schizophrenia risk variants and their cis-target genes. This study highlights ASoC as a functional mechanism of noncoding neuropsychiatric risk variants, providing a powerful framework for identifying disease causal variants and genes.Entities:
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Year: 2020 PMID: 32732423 DOI: 10.1126/science.aay3983
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728