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Identification of genetic variation influencing metformin response in a multi-ancestry genome-wide association study in the Diabetes Prevention Program (DPP)

Authors :
Diabetes Prevention Program Research Group
Jose C. Florez
Toni I. Pollin
William C. Knowler
Steven E. Kahn
Robert L. Hanson
Paul W. Franks
L. Keoki Williams
Shujie Xiao
Adriana M. Hung
Ayush Giri
Kathleen M. Giacomini
Ewan R. Pearson
Sook Wah Yee
Adem Y. Dawed
Qing Pan
Josep M. Mercader
Maegan Harden
Jennifer N. Todd
Ling Chen
Shylaja Srinivasan
Kathleen A. Jablonski
James A. Perry
Josephine Li
Publication Year :
2023
Publisher :
American Diabetes Association, 2023.

Abstract

Genome-wide significant loci for metformin response in type 2 diabetes reported elsewhere have not replicated in the Diabetes Prevention Program (DPP). To assess pharmacogenetic interactions in pre-diabetes, we conducted a genome-wide association study (GWAS) in the DPP. Cox proportional hazards models tested associations with diabetes incidence in metformin (MET, n=876) and placebo (PBO, n=887) arms. Multiple linear regression assessed association with one-year change in metformin-related quantitative traits, adjusted for baseline trait, age, sex, and 10 ancestry principal components. We tested for gene-by-treatment interaction. No significant associations emerged for diabetes incidence. We identified four genome-wide significant variants after correcting for correlated traits (pENOSF1 (minor allele frequency [MAF]AFR=0.07, MAFEUR=0.002) was associated with an increase in % glycated hemoglobin (per minor allele β=0.39 [95% CI 0.28, 0.50], p=2.8×10-12). Rs145591055 near OMSR (MAF=0.10 in American Indians), was associated with weight loss (kg) (per G allele β=-7.55 [95% CI -9.88, -5.22], p=3.2×10-10) in MET. Neither variant was significant in PBO; gene-by-treatment interaction was significant for both variants (p(G×T)

Details

Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....de6390e02ff019f014b64ab35178d8cd
Full Text :
https://doi.org/10.2337/figshare.21719837