A Two-Stage Study Identifies Two Novel Polymorphisms in Affecting Metformin Response in Chinese Type 2 Diabetes Patients

Overview

Journal Pharmgenomics Pers Med

Publisher Dove Medical Press

Date 2021 Jun 30

PMID 34188521

Citations 3

Authors

Di Xiao

Jun-Yan Liu

Si-Min Zhang

Rang-Ru Liu

Ji-Ye Yin

Xue-Yao Han

Xi Li

Wei Zhang

Xiao-Ping Chen

Hong-Hao Zhou

Li-Nong Ji

Zhao-Qian Liu

Affiliations

Soon will be listed here.

Abstract

Objective: Individual differences in glycemic response to metformin in antidiabetic treatment exist widely. Although some associated genetic variations have been discovered, they still cannot accurately predict metformin response. In the current study, we set out to investigate novel genetic variants affecting metformin response in Chinese type 2 diabetes (T2D) patients.

Methods: A two-stage study enrolled 500 T2D patients who received metformin, glibenclamide or a combination of both were recruited from 2009 to 2012 in China. Change of HbA, adjusted by clinical covariates, was used to evaluate glycemic response to metformin. Selected single nucleotide polymorphisms (SNPs) were genotyped using the Infinium iSelect and/or Illumina GoldenGate genotyping platform. A linear regression model was used to evaluate the association between SNPs and response.

Results: A total of 3739 SNPs were screened in Stage 1, of which 50 were associated with drug response. Except for one genetic variant preferred to affect glibenclamide, the remaining SNPs were subsequently verified in Stage 2, and two SNPs were successfully validated. These were rs2727528 (discovery group: β=-0.212, =0.046; validation group: β=-0.269, =0.028) and rs1105842 (discovery group: β=0.205, =0.048; validation group: β=0.273, =0.025). C allele carriers of rs2727528 and C allele carriers of rs1105842 would have a larger difference of HbA level when using metformin.

Conclusion: Two variants rs2727528 and rs1105842 in , encoding γ2 subunit of AMP-activated protein kinase (AMPK), were found to be associated with metformin response in Chinese T2D patients. These findings may provide some novel information for personalized pharmacotherapy of metformin in China.

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