Association of the Reduced Function Met420del Polymorphism of SLC22A1 with Metformin-Induced Gastrointestinal Intolerance in Ethiopian Patients with Type 2 Diabetes Mellitus

Abraham Degaga, Sisay Sirgu, Hasniza Zaman Huri, Maw Shin Sim, Navin Kumar Loganadan, Tedla Kebede, Birhanemeskel Tegene, Ephrem Engidawork, Workineh Shibeshi
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Abstract

Background: Despite its widespread use and favored profile, there are extensive variations in the treatment outcome of metformin therapy. Furthermore, studies reported that the inter-individual variability in the occurrence of metformin treatment associated side effects were related to the differences in individual genetic profiles. Thus, this study aimed to evaluate whether the reduced function methionine deletion at codon 420 (Met420del) variant of SLC22A1 (rs72552763) is associated with metformin induced gastrointestinal intolerance in Ethiopian patients with type 2 diabetes mellitus (T2DM).
Patients and Methods: A retrospective observational study was conducted on 47 T2DM patients on metformin treatment for < 3 years to assess the association of SLC22A1 (rs72552763) polymorphism with metformin induced gastrointestinal intolerance. Accordingly, 24 metformin tolerant and 23 metformin intolerant individuals with T2DM were recruited. Genotyping of rs72552763 was performed using TaqMan® Drug Metabolism Enzyme Genotyping Assay and its association to metformin induced gastrointestinal intolerance was assessed based on switching to a new class of glucose lowering agents or failure to up titrate dose due to metformin induced gastrointestinal intolerance. Chi-square, logistic regression and Mann–Whitney statistical tests were used as appropriate. Statistical significance was set at p < 0.05.
Results: In our study, no significant association was observed between rs72552763 and metformin induced gastrointestinal intolerance. We found that the female gender and physical inactivity were risk factors for metformin gastrointestinal intolerance.
Conclusion: Our study found that the Met420del variant of SLC22A1 (rs72552763) was not associated with metformin induced gastrointestinal intolerance in Ethiopian patients with T2DM. This is the study first to investigate the association of rs72552763 with metformin intolerance in the Ethiopian population with T2DM. However, the findings need to be cautiously interpreted given the relatively small sample size. In addition, a more complete investigation of SLC22A1 variants would be required to fully assess the effect of the gene on metformin induced gastrointestinal intolerance as several variants with a more severe loss of function have been described.

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埃塞俄比亚 2 型糖尿病患者 SLC22A1 功能降低 Met420del 多态性与二甲双胍诱发的胃肠道不耐受的关系
背景:尽管二甲双胍被广泛使用,且备受青睐,但其治疗效果却存在很大差异。此外,有研究报告称,二甲双胍治疗相关副作用发生的个体间差异与个体遗传特征的差异有关。因此,本研究旨在评估埃塞俄比亚 2 型糖尿病(T2DM)患者中,SLC22A1(rs72552763)第 420 号密码子(Met420del)蛋氨酸功能缺失变异是否与二甲双胍诱导的胃肠道不耐受有关:对47名接受二甲双胍治疗3年的T2DM患者进行了一项回顾性观察研究,以评估SLC22A1(rs72552763)多态性与二甲双胍诱导的胃肠道不耐受的相关性。因此,研究人员招募了 24 名二甲双胍耐受和 23 名二甲双胍不耐受的 T2DM 患者。使用TaqMan®药物代谢酶基因分型分析法对rs72552763进行基因分型,并根据二甲双胍引起的胃肠道不耐受而改用新的降糖药物或剂量滴定失败来评估其与二甲双胍引起的胃肠道不耐受的关系。根据情况使用了卡方、逻辑回归和曼-惠特尼统计检验。统计显著性设定为 p < 0.05:在我们的研究中,没有观察到 rs72552763 与二甲双胍引起的胃肠道不耐受之间有明显的关联。我们发现,女性性别和缺乏运动是二甲双胍胃肠道不耐受的风险因素:我们的研究发现,在埃塞俄比亚的 T2DM 患者中,SLC22A1 的 Met420del 变异(rs72552763)与二甲双胍诱发的胃肠道不耐受无关。这是首次在埃塞俄比亚 T2DM 患者中研究 rs72552763 与二甲双胍不耐受的关系。然而,由于样本量相对较小,因此需要谨慎解释研究结果。此外,还需要对 SLC22A1 变体进行更全面的调查,以全面评估该基因对二甲双胍诱发的胃肠道不耐受的影响,因为有几个功能丧失更严重的变体已被描述过。
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