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Non-coding de novo mutations in chromatin interactions are implicated in autism spectrum disorder

Authors
Kim, Il BinLee, TaeyeopLee, JunehawkKim, JonghunLee, SuhoKoh, In GyeongKim, Jae HyunAn, Joon-YongLee, HyunseongKim, Woo KyeongJu, Young SeokCho, YongseongYu, Seok JongKim, Soon AeOh, MiaeHan, Dong WookKim, EunjoonChoi, Jung KyoonYoo, Hee JeongLee, Jeong Ho
Issue Date
2022
Publisher
SPRINGERNATURE
Citation
MOLECULAR PSYCHIATRY
Indexed
SCIE
SCOPUS
Journal Title
MOLECULAR PSYCHIATRY
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/142853
DOI
10.1038/s41380-022-01697-2
ISSN
1359-4184
Abstract
Three-dimensional chromatin interactions regulate gene expressions. The significance of de novo mutations (DNMs) in chromatin interactions remains poorly understood for autism spectrum disorder (ASD). We generated 813 whole-genome sequences from 242 Korean simplex families to detect DNMs, and identified target genes which were putatively affected by non-coding DNMs in chromatin interactions. Non-coding DNMs in chromatin interactions were significantly involved in transcriptional dysregulations related to ASD risk. Correspondingly, target genes showed spatiotemporal expressions relevant to ASD in developing brains and enrichment in biological pathways implicated in ASD, such as histone modification. Regarding clinical features of ASD, non-coding DNMs in chromatin interactions particularly contributed to low intelligence quotient levels in ASD probands. We further validated our findings using two replication cohorts, Simons Simplex Collection (SSC) and MSSNG, and showed the consistent enrichment of non-coding DNM-disrupted chromatin interactions in ASD probands. Generating human induced pluripotent stem cells in two ASD families, we were able to demonstrate that non-coding DNMs in chromatin interactions alter the expression of target genes at the stage of early neural development. Taken together, our findings indicate that non-coding DNMs in ASD probands lead to early neurodevelopmental disruption implicated in ASD risk via chromatin interactions.
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