A population study of clinically actionable genetic variation affecting drug response from the Middle East

Author:

Jithesh Puthen VeettilORCID,Abuhaliqa Mohammed,Syed Najeeb,Ahmed IkhlakORCID,El Anbari Mohammed,Bastaki Kholoud,Sherif Shimaa,Umlai Umm-KulthumORCID,Jan Zainab,Gandhi Geethanjali,Manickam Chidambaram,Selvaraj SenthilORCID,George Chinnu,Bangarusamy Dhinoth,Abdel-latif Rania,Al-Shafai Mashael,Tatari-Calderone Zohreh,Estivill Xavier,Pirmohamed MunirORCID,Abdel-latif Rania,Saqri Tariq Abu,Zaid Tariq Abu,Afifi Nahla,Al-Ali Rashid,Al-Khodor Souhaila,Al-Muftah Wadha,Al-Sarraj Yasser,Albagha Omar,Alkhayat Eiman,Alkuwari Fatima,Almabrazi Hakeem,Alshafai Mashael,Althani Asmaa,Alvi Muhammad,Badii Ramin,Badji Radja,Chouchane Lotfi,Darwish Dima,El Khouly Ahmed,Ennaifar Maryem,Estivill Xavier,Fadl Tasnim,Fakhro Khalid,Fethnou Eleni,Hamza Mehshad,Ismail Said I.,Jithesh Puthen V.,Khatib Mohammedhusen,Liu Wei,Lorenz Stephan,Mbarek Hamdi,Mokrab Younes,Pathare Tushar,Poolat Shafeeq,Qafoud Fatima,Vempalli Fazulur Rehaman,Saad Chadi,Suhre Karsten,Syed Najeeb,Tatari Zohreh,Temanni Ramzi,Tomei Sara,Yasin Heba,

Abstract

AbstractClinical implementation of pharmacogenomics will help in personalizing drug prescriptions and alleviate the personal and financial burden due to inefficacy and adverse reactions to drugs. However, such implementation is lagging in many parts of the world, including the Middle East, mainly due to the lack of data on the distribution of actionable pharmacogenomic variation in these ethnicities. We analyzed 6,045 whole genomes from the Qatari population for the distribution of allele frequencies of 2,629 variants in 1,026 genes known to affect 559 drugs or classes of drugs. We also performed a focused analysis of genotypes or diplotypes of 15 genes affecting 46 drugs, which have guidelines for clinical implementation and predicted their phenotypic impact. The allele frequencies of 1,320 variants in 703 genes affecting 299 drugs or class of drugs were significantly different between the Qatari population and other world populations. On average, Qataris carry 3.6 actionable genotypes/diplotypes, affecting 13 drugs with guidelines for clinical implementation, and 99.5% of the individuals had at least one clinically actionable genotype/diplotype. Increased risk of simvastatin-induced myopathy could be predicted in ~32% of Qataris from the diplotypes of SLCO1B1, which is higher compared to many other populations, while fewer Qataris may need tacrolimus dosage adjustments for achieving immunosuppression based on the CYP3A5 diplotypes compared to other world populations. Distinct distribution of actionable pharmacogenomic variation was also observed among the Qatari subpopulations. Our comprehensive study of the distribution of actionable genetic variation affecting drugs in a Middle Eastern population has potential implications for preemptive pharmacogenomic implementation in the region and beyond.

Publisher

Springer Science and Business Media LLC

Subject

Genetics (clinical),Genetics,Molecular Biology

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