Single Nucleotide Variants as Proxies for in Native American Populations.

Front Pharmacol

Coordenação de Pesquisa, Instituto Nacional de Câncer, Rio de Janeiro, Brazil.

Published: April 2022

AI Article Synopsis

  • - Carbamazepine can cause skin hypersensitivity reactions linked to certain human leukocyte antigens (HLAs), and previous studies have identified specific genetic variants (rs1061235 and rs17179220) with predictive potential for these reactions in various populations.
  • - The research examined how well these genetic variants serve as predictive markers in diverse groups of individuals with Native American ancestry, which are often overlooked in pharmacogenomic research.
  • - The findings showed that while these variants performed well in some populations, they aren't consistently reliable across all Native American groups, indicating they may not be the best proxies for predicting adverse reactions to carbamazepine.

Article Abstract

Carbamazepine triggers dermatologic hypersensitivity reactions, associated with specific human leukocyte antigens (HLAs), especially and Previous efforts to identify single nucleotide variants (SNVs) with high predictive value as HLA proxies, revealed that rs1061235 and rs17179220 fulfill these requirements for in some but not all populations. Herein we explored the predictive performance of rs1061235 and rs17179220 as tags in populations of Native American ancestry, which are largely underrepresented in pharmacogenomic studies. The study cohorts comprised the overall Admixed American superpopulation of the 1000 Genomes Project (1 KG_AMR), a subcohort of individuals with predominant Native American ancestry (1 KG_NAT), the Native American population of the Human Genome Diversity Project (HGDP), plus Kaingang (KRC) and Guarani (GRC and GKW) adults from indigenous reservation areas in Brazil. The diversity of cohorts is reflected in the range of frequencies of (0.02-0.65), rs1061235 (0.03-0.13) and rs17179220 (0.12-0.66), as well as in the predictive performance of these SNVs as proxies. NPV (negative predictive value), the metric of primary interest for pharmacogenetic-informed carbamazepine prescription was maximal (NPV = 1.0) for both SNVs in 1 KG_AMR and 1 KG_NAT, for rs17179220, but not rs1061235 (NPV = 0.91) in HGDP, and for rs17179220 in GWK, but not GRC (NPV = 0.88) or KRC (NPV = 0.80). Collectively, the data support the notion that rs1061235 and rs17179220 are not optimal proxies for across populations of Native American ancestry.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9046591PMC
http://dx.doi.org/10.3389/fphar.2022.849136DOI Listing

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