학술논문
Genomic architecture of autism spectrum disorder in Qatar: The BARAKA-Qatar Study
Document Type
article
Author
Mona Abdi; Elbay Aliyev; Brett Trost; Muhammad Kohailan; Waleed Aamer; Najeeb Syed; Rulan Shaath; Geethanjali Devadoss Gandhi; Worrawat Engchuan; Jennifer Howe; Bhooma Thiruvahindrapuram; Melissa Geng; Joe Whitney; Amira Syed; Jyothi Lakshmi; Sura Hussein; Najwa Albashir; Amal Hussein; Ilaria Poggiolini; Saba F. Elhag; Sasirekha Palaniswamy; Marios Kambouris; Maria de Fatima Janjua; Mohamed O. El Tahir; Ahsan Nazeer; Durre Shahwar; Muhammad Waqar Azeem; Younes Mokrab; Nazim Abdel Aati; Ammira Akil; Stephen W. Scherer; Madeeha Kamal; Khalid A. Fakhro
Source
Genome Medicine, Vol 15, Iss 1, Pp 1-16 (2023)
Subject
Language
English
ISSN
1756-994X
Abstract
Abstract Background Autism spectrum disorder (ASD) is a neurodevelopmental condition characterized by impaired social and communication skills, restricted interests, and repetitive behaviors. The prevalence of ASD among children in Qatar was recently estimated to be 1.1%, though the genetic architecture underlying ASD both in Qatar and the greater Middle East has been largely unexplored. Here, we describe the first genomic data release from the BARAKA-Qatar Study—a nationwide program building a broadly consented biorepository of individuals with ASD and their families available for sample and data sharing and multi-omics research. Methods In this first release, we present a comprehensive analysis of whole-genome sequencing (WGS) data of the first 100 families (372 individuals), investigating the genetic architecture, including single-nucleotide variants (SNVs), copy number variants (CNVs), tandem repeat expansions (TREs), as well as mitochondrial DNA variants (mtDNA) segregating with ASD in local families. Results Overall, we identify potentially pathogenic variants in known genes or regions in 27 out of 100 families (27%), of which 11 variants (40.7%) were classified as pathogenic or likely-pathogenic based on American College of Medical Genetics (ACMG) guidelines. Dominant variants, including de novo and inherited, contributed to 15 (55.6%) of these families, consisting of SNVs/indels (66.7%), CNVs (13.3%), TREs (13.3%), and mtDNA variants (6.7%). Moreover, homozygous variants were found in 7 families (25.9%), with a sixfold increase in homozygous burden in consanguineous versus non-consanguineous families (13.6% and 1.8%, respectively). Furthermore, 28 novel ASD candidate genes were identified in 20 families, 23 of which had recurrent hits in MSSNG and SSC cohorts. Conclusions This study illustrates the value of ASD studies in under-represented populations and the importance of WGS as a comprehensive tool for establishing a molecular diagnosis for families with ASD. Moreover, it uncovers a significant role for recessive variation in ASD architecture in consanguineous settings and provides a unique resource of Middle Eastern genomes for future research to the global ASD community.