The contribution of de novo coding mutations to autism spectrum disorder

Ivan Iossifov,Brian J. O'Roak,Stephan J. Sanders,Michael Ronemus,Niklas Krumm,Dan Levy,Holly A. F. Stessman,Kali Witherspoon,Laura Vives,Karynne E. Patterson,Joshua D. Smith,Bryan W. Paeper,Deborah A. Nickerson,Jeanselle Dea,Shan Dong,Luis Gonzalez,Jeffrey D. Mandell,Shrikant Mane,Michael T. Murtha,Catherine A.W. Sullivan,Michael F. Walker,Zainulabedin Waqar,Liping Wei,A. Jeremy Willsey,Boris Yamrom,Yoon Ha Lee,Ewa A. Grabowska,Ertugrul Dalkic,Zihua Wang,Steven Marks,Peter Andrews,Anthony Leotta,Jude Kendall,Inessa Hakker,Julie Rosenbaum,Beicong Ma,Linda Rodgers,Jennifer Troge,Giuseppe Narzisi,Seungtai Yoon,Michael C. Schatz,Kenny Ye,W. Richard McCombie,Jay Shendure,Evan E. Eichler,Matthew W. State,Michael Wigler

The contribution of de novo coding mutations to autism spectrum disorder

2014

Family-based exome sequencing in a large autism study has identified 27 high-confidence gene targets and accurately estimates the contribution of both de novo gene-disrupting and missense mutations to the incidence of simplex autism, with target genes in affected females overlapping those in males of lower but not higher IQ; targets also overlap known targets for intellectual disability and schizophrenia, and are enriched for chromatin modifiers, FMRP-associated genes and embryonically expressed genes.

Keywords:

Autism spectrum disorder
Exome
Exome sequencing
Autism
Missense mutation
Gene
Intellectual disability
Mutation
Genetics
Biology
Bioinformatics
Childhood disintegrative disorder
SYNGAP1

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