Pharmacogenomic variation in the Malagasy population: implications for the antimalarial drug primaquine metabolism.
Estee Y CramerJacquelaine BartlettErnest R ChanAndrea GaedigkArsene C RatsimbasoaRajeev K MehlotraScott M WilliamsPeter A ZimmermanPublished in: Pharmacogenomics (2023)
Aim: Antimalarial primaquine (PQ) eliminates liver hypnozoites of Plasmodium vivax. CYP2D6 gene variation contributes to PQ therapeutic failure. Additional gene variation may contribute to PQ efficacy. Information on pharmacogenomic variation in Madagascar, with vivax malaria and a unique population admixture, is scanty. Methods: The authors performed genome-wide genotyping of 55 Malagasy samples and analyzed data with a focus on a set of 28 pharmacogenes most relevant to PQ. Results: Mainly, the study identified 110 coding or splicing variants, including those that, based on previous studies in other populations, may be implicated in PQ response and copy number variation, specifically in chromosomal regions that contain pharmacogenes. Conclusion: With this pilot information, larger genome-wide association analyses with PQ metabolism and response are substantially more feasible.
Keyphrases
- copy number
- genome wide
- mitochondrial dna
- dna methylation
- plasmodium falciparum
- genome wide association
- clinical decision support
- emergency department
- randomized controlled trial
- high throughput
- gene expression
- health information
- machine learning
- social media
- electronic health record
- drug induced
- genome wide identification