Using whole-exome sequencing to identify inherited causes of autism

Timothy W Yu; Maria H Chahrour; Michael E Coulter; Sarn Jiralerspong; Kazuko Okamura-Ikeda; Bulent Ataman; Klaus Schmitz-Abe; David A Harmin; Mazhar Adli; Athar N Malik; Alissa M D'Gama; Elaine T Lim; Stephan J Sanders; Ganesh H Mochida; Jennifer N Partlow; Christine M Sunu; Jillian M Felie; Jacqueline Rodriguez; Ramzi H Nasir; Janice Ware; Robert M Joseph; R Sean Hill; Benjamin Y Kwan; Muna Al-Saffar; Nahit M Mukaddes; Asif Hashmi; Soher Balkhy; Generoso G Gascon; Fuki M Hisama; Elaine LeClair; Annapurna Poduri; Ozgur Oner; Samira Al-Saad; Sadika A Al-Awadi; Laila Bastaki; Tawfeg Ben-Omran; Ahmad S Teebi; Lihadh Al-Gazali; Valsamma Eapen; Christine R Stevens; Leonard Rappaport; Stacey B Gabriel; Kyriacos Markianos; Matthew W State; Michael E Greenberg; Hisaaki Taniguchi; Nancy E Braverman; Eric M Morrow; Christopher A Walsh

doi:10.1016/j.neuron.2012.11.002

Using whole-exome sequencing to identify inherited causes of autism

Neuron. 2013 Jan 23;77(2):259-73. doi: 10.1016/j.neuron.2012.11.002.

Authors

Timothy W Yu¹, Maria H Chahrour, Michael E Coulter, Sarn Jiralerspong, Kazuko Okamura-Ikeda, Bulent Ataman, Klaus Schmitz-Abe, David A Harmin, Mazhar Adli, Athar N Malik, Alissa M D'Gama, Elaine T Lim, Stephan J Sanders, Ganesh H Mochida, Jennifer N Partlow, Christine M Sunu, Jillian M Felie, Jacqueline Rodriguez, Ramzi H Nasir, Janice Ware, Robert M Joseph, R Sean Hill, Benjamin Y Kwan, Muna Al-Saffar, Nahit M Mukaddes, Asif Hashmi, Soher Balkhy, Generoso G Gascon, Fuki M Hisama, Elaine LeClair, Annapurna Poduri, Ozgur Oner, Samira Al-Saad, Sadika A Al-Awadi, Laila Bastaki, Tawfeg Ben-Omran, Ahmad S Teebi, Lihadh Al-Gazali, Valsamma Eapen, Christine R Stevens, Leonard Rappaport, Stacey B Gabriel, Kyriacos Markianos, Matthew W State, Michael E Greenberg, Hisaaki Taniguchi, Nancy E Braverman, Eric M Morrow, Christopher A Walsh

Affiliation

¹ Division of Genetics, Department of Medicine, Boston Children's Hospital, Boston, MA 02115, USA. timothy.yu@childrens.harvard.edu

Abstract

Despite significant heritability of autism spectrum disorders (ASDs), their extreme genetic heterogeneity has proven challenging for gene discovery. Studies of primarily simplex families have implicated de novo copy number changes and point mutations, but are not optimally designed to identify inherited risk alleles. We apply whole-exome sequencing (WES) to ASD families enriched for inherited causes due to consanguinity and find familial ASD associated with biallelic mutations in disease genes (AMT, PEX7, SYNE1, VPS13B, PAH, and POMGNT1). At least some of these genes show biallelic mutations in nonconsanguineous families as well. These mutations are often only partially disabling or present atypically, with patients lacking diagnostic features of the Mendelian disorders with which these genes are classically associated. Our study shows the utility of WES for identifying specific genetic conditions not clinically suspected and the importance of partial loss of gene function in ASDs.

Publication types

Case Reports
Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Animals
Autistic Disorder / diagnosis*
Autistic Disorder / genetics*
Cells, Cultured
Child
Child, Preschool
Cohort Studies
Exome / genetics*
Female
Genome-Wide Association Study / methods*
Humans
Male
Pedigree
Rats
Sequence Analysis, DNA / methods
Young Adult

Abstract

Publication types

MeSH terms

Grants and funding