Targeted next-generation sequencing of genes involved in Warfarin Pharmacodynamics and pharmacokinetics pathways using the Saudi Warfarin Pharmacogenetic study (SWAP).

Maha Al Ammari Bader Almuzzaini Khalid Al Sulaiman Mohammed AlBalwi Khizra Sultana Ibrahim B Alabdulkareem Nada S Almakhlafi Anoud Al Humoud Mohammed Waheeby Munee Balla Asma Al Shehri Adel Alharf Jahad Alghamdi

Pharmacogenomics J

Saudi Food and Drug Authority, Drug Sector, Riyadh, Saudi Arabia.

Published: July 2023

Warfarin is a widely used anticoagulant requiring careful monitoring due to its narrow therapeutic index, influenced by genetic and individual factors.
This study utilized next-generation sequencing to analyze 786 patients, identifying 710 genetic variants linked to warfarin dosage.
Findings highlight novel, population-specific genetic variants associated with warfarin response, underscoring the need for tailored dosing algorithms rather than a one-size-fits-all approach.

Background: Warfarin is an oral anticoagulant commonly used for treatment and prophylaxis against thromboembolic events. Warfarins's narrow therapeutic index window is one of the main challenges in clinical practice; thus, it requires frequent monitoring and dose adjustment to maintain patients' therapeutic range. Warfarin dose variation and response are attributed to several inter-and intra-individuals factors, including genetic variants in enzymes involved in warfarin pharmacokinetics (PK) and pharmacodynamics (PD) pathways. Thus, we aim to utilize the next-generation sequencing (NGS) approach to identify rare and common genetic variants that might be associated with warfarin responsiveness.

Method And Results: A predesigned NGS panel that included 16 genes involved in Warfarin PK/PD pathways was used to sequence 786 patients from the Saudi Warfarin Pharmacogenetic Cohort (SWAP). Identified variants were annotated using several annotation tools to identify the pathogenicity and allele frequencies of these variants. We conducted variants-level association tests with warfarin dose. We identified 710 variants within the sequenced genes; 19% were novel variants, with the vast majority being scarce variants. The genetic association tests showed that VKORC1 (rs9923231, and rs61742245), CYP2C9 (rs98332238, rs9332172, rs1057910, rs9332230, rs1799853, rs1057911, and rs9332119), CYP2C19 (rs28399511, and rs3758581), and CYP2C8 (rs11572080 and rs10509681) were significantly associated with warfarin weekly dose. Our model included genetics, and non-genetic factors explained 40.1% of warfarin dose variation.

Conclusion: The study identifies novel variants associated with warfarin dose in the Saudi population. These variants are more likely to be population-specific variants, suggesting that population-specific studies should be conducted before adopting a universal warfarin genotype-guided dosing algorithm.

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http://dx.doi.org/10.1038/s41397-023-00300-3	DOI Listing

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