| Literature DB >> 28803920 |
Marc P Forrest1, Hanwen Zhang2, Winton Moy2, Heather McGowan3, Catherine Leites2, Leonardo E Dionisio1, Zihui Xu3, Jianxin Shi4, Alan R Sanders5, William J Greenleaf6, Chad A Cowan7, Zhiping P Pang3, Pablo V Gejman5, Peter Penzes8, Jubao Duan9.
Abstract
Most disease variants lie within noncoding genomic regions, making their functional interpretation challenging. Because chromatin openness strongly influences transcriptional activity, we hypothesized that cell-type-specific open chromatin regions (OCRs) might highlight disease-relevant noncoding sequences. To investigate, we mapped global OCRs in neurons differentiating from hiPSCs, a cellular model for studying neurodevelopmental disorders such as schizophrenia (SZ). We found that the OCRs are highly dynamic and can stratify GWAS-implicated SZ risk variants. Of the more than 3,500 SZ-associated variants analyzed, we prioritized ∼100 putatively functional ones located in neuronal OCRs, including rs1198588, at a leading risk locus flanking MIR137. Excitatory neurons derived from hiPSCs with CRISPR/Cas9-edited rs1198588 or a rare proximally located SZ risk variant showed altered MIR137 expression, dendrite arborization, and synapse maturation. Our study shows that noncoding disease variants in OCRs can affect neurodevelopment, and that analysis of open chromatin regions can help prioritize functionally relevant noncoding variants identified by GWAS.Entities:
Keywords: ATAC-seq; CRISPR/Cas9; GWAS; MIR137; hiPSC; neurodevelopment; noncoding; open chromatin; schizophrenia; synapse
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Year: 2017 PMID: 28803920 PMCID: PMC5591074 DOI: 10.1016/j.stem.2017.07.008
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633