Targeted massively parallel sequencing of autism spectrum disorder-associated genes in a case control cohort reveals rare loss-of-function risk variants

Anthony J. Griswold,Nicole Dueker,Derek Van Booven,Joseph A. Rantus,James Jaworski,Susan Slifer,Michael A. Schmidt,William Hulme,Ioanna Konidari,Patrice L. Whitehead,Michael L. Cuccaro,Eden R. Martin,Jonathan L. Haines,John R. Gilbert,John P. Hussman,Margaret A. Pericak-Vance

Targeted massively parallel sequencing of autism spectrum disorder-associated genes in a case control cohort reveals rare loss-of-function risk variants

2015

Anthony J. Griswold
Nicole Dueker
Derek Van Booven
Joseph A. Rantus
James Jaworski
Susan Slifer
Michael A. Schmidt
William Hulme
Ioanna Konidari
Patrice L. Whitehead
Michael L. Cuccaro
Eden R. Martin
Jonathan L. Haines
John R. Gilbert
John P. Hussman
Margaret A. Pericak-Vance

Background Autism spectrum disorder (ASD) is highly heritable, yet genome-wide association studies (GWAS), copy number variation screens, and candidate gene association studies have found no single factor accounting for a large percentage of genetic risk. ASD trio exome sequencing studies have revealed genes with recurrent de novo loss-of-function variants as strong risk factors, but there are relatively few recurrently affected genes while as many as 1000 genes are predicted to play a role. As such, it is critical to identify the remaining rare and low-frequency variants contributing to ASD.

Keywords:

Genetic association
Genetics
Massive parallel sequencing
Exome sequencing
Autism spectrum disorder
Molecular medicine
Candidate gene
Psychology
Copy-number variation
Genome-wide association study
Loss function
Medicine

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