Actionable genomic variants in 6045 participants from the Qatar Genome Program
Date
2021-08-24Author
Elfatih, AmalMifsud, Borbala
Syed, Najeeb
Badii, Ramin
Mbarek, Hamdi
Abbaszadeh, Fatemeh
Estivill, Xavier
Ismail, Said
Al-Muftah, Wadha
Badji, Radja
Darwish, Dima
Fadl, Tasnim
Yasin, Heba
Ennaifar, Maryem
Abdel-latif, Rania
Alkuwari, Fatima
Alvi, Muhammad
Sarraj, Yasser Al
Saad, Chadi
Althani, Asmaa
Fethnou, Eleni
Qafoud, Fatima
Alkhayat, Eiman
Afifi, Nahla
Tomei, Sara
Liu, Wei
Lorenz, Stephan
Almabrazi, Hakeem
Vempalli, Fazulur Rehaman
Temanni, Ramzi
Saqri, Tariq Abu
Khatib, Mohammedhusen
Hamza, Mehshad
Zaid, Tariq Abu
El Khouly, Ahmed
Pathare, Tushar
Poolat, Shafeeq
Al-Ali, Rashid
Albagha, Omar M.E.
Al-Khodor, Souhaila
Alshafai, Mashael
Chouchane, Lotfi
Fakhro, Khalid
Mokrab, Younes
Puthen, Jithesh V.
Suhre, Karsten
Tatari, Zohreh
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Show full item recordAbstract
In a clinical setting, DNA sequencing can uncover findings unrelated to the purpose of genetic evaluation. The American College of Medical Genetics and Genomics (ACMG) recommends the evaluation and reporting of 59 genes from clinic genomic sequencing. While the prevalence of secondary findings is available from large population studies, these data lack Arab and other Middle Eastern populations. The Qatar Genome Program (QGP) generates whole-genome sequencing (WGS) data and combines it with phenotypic information to create a comprehensive database for studying the Qatari and wider Arab and Middle Eastern populations at the molecular level. This study identified and analyzed medically actionable variants in the 59 ACMG genes using WGS data from 6045 QGP participants. Our results identified a total of 60 pathogenic and likely pathogenic variants in 25 ACMG genes in 141 unique individuals. Overall, 2.3% of the QGP sequenced participants carried a pathogenic or likely pathogenic variant in one of the 59 ACMG genes. We evaluated the QGP phenotype-genotype association of additional nonpathogenic ACMG variants. These variants were found in patients from the Hamad Medical Corporation or reported incidental findings data in Qatar. We found a significant phenotype association for two variants, c.313+3A>C in LDLR, and c.58C>T (p.Gln20*) in the TPM1.
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