Genome-wide de novo risk score implicates promoter variation in autism spectrum disorder.

Science

Authors	Joon-Yong An Kevin Lin Lingxue Zhu Donna Werling Shan Dong Harrison Brand Harold Wang Xuefang Zhao Grace Schwartz Ryan Collins Benjamin Currall Claudia Dastmalchi Jeanselle Dea Clif Duhn Michael Gilson Lambertus Klei Lindsay Liang Eirene Markenscoff-Papadimitriou Sirisha Pochareddy Nadav Ahituv Joseph Buxbaum Hilary Coon Mark Daly Young Kim Gabor Marth Benjamin Neale Aaron Quinlan John Rubenstein Nenad Sestan Matthew State A Jeremy Willsey Michael Talkowski Bernie Devlin Kathryn Roeder Stephan Sanders
Keywords	Humans Mutation Binding Sites Conserved Sequence Transcription Factors Genetic Variation Promoter Regions, Genetic DNA Mutational Analysis Genetic Loci Pedigree Autism Spectrum Disorder Risk
Abstract	Whole-genome sequencing (WGS) has facilitated the first genome-wide evaluations of the contribution of de novo noncoding mutations to complex disorders. Using WGS, we identified 255,106 de novo mutations among sample genomes from members of 1902 quartet families in which one child, but not a sibling or their parents, was affected by autism spectrum disorder (ASD). In contrast to coding mutations, no noncoding functional annotation category, analyzed in isolation, was significantly associated with ASD. Casting noncoding variation in the context of a de novo risk score across multiple annotation categories, however, did demonstrate association with mutations localized to promoter regions. We found that the strongest driver of this promoter signal emanates from evolutionarily conserved transcription factor binding sites distal to the transcription start site. These data suggest that de novo mutations in promoter regions, characterized by evolutionary and functional signatures, contribute to ASD.
Year of Publication	2018
Journal	Science
Volume	362
Issue	6420
Date Published	2018 12 14
ISSN	1095-9203
DOI	10.1126/science.aat6576
PubMed ID	30545852
PubMed Central ID	PMC6432922
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