Division of Endocrine and Metabolic Diseases, Center for Biomedical Science, Korea National Institute of Health, Cheongwon-gun, Chungcheongbuk-do, 363-951, South Korea.
Sci Rep. 2021 Feb 25;11(1):4729. doi: 10.1038/s41598-021-84179-9.
Chronic alcohol consumption is known to be associated with type 2 diabetes (T2D), which is developed by two underlying mechanisms, β-cell dysfunction and insulin resistance. Identification of genetic variants in association with the development of T2D may help explain the genetic risk factors of T2D. In this study, we tried to find out some genetic variations, which interact with alcohol consumption and also are associated with β-cell function through 12 year's follow-up study in Korean population. We performed a genotype association study using the community-based Ansung-Ansan Cohort data (baseline n = 3120; follow-up n = 433). Genotype association analyses of the baseline data showed that alcohol consumption is associated with the decreases of blood insulin levels and insulin secretion in participants with the KCNJ11 rs5219 risk allele. Moreover, multivariate logistic regression analyses revealed that the risk allele group is vulnerable to impairment of β-cell function in response to alcohol consumption (OR 1.450; 95% CI 1.061-1.982). Furthermore, 12-year' follow-up results showed that alcohol consumption synergistically decreases insulin secretion in participants with KCNJ11 rs5219 risk alleles. Our findings demonstrate that the KCNJ11 rs5219 risk allele in combination with alcohol consumption could be a potential risk factor of β-cell dysfunction. We hope that this new findings could be helpful to further understand the development of T2D depending on individual genetic background in association with alcohol consumption.
慢性酒精摄入与 2 型糖尿病(T2D)有关,T2D 的发生涉及两种潜在机制,即β细胞功能障碍和胰岛素抵抗。鉴定与 T2D 发展相关的遗传变异可能有助于解释 T2D 的遗传风险因素。在这项研究中,我们试图通过对韩国人群进行 12 年的随访研究,找出一些与酒精摄入相互作用并与β细胞功能相关的遗传变异。我们使用基于社区的安山-安山队列数据(基线 n=3120;随访 n=433)进行了基因型关联研究。基线数据的基因型关联分析表明,酒精摄入与具有 KCNJ11 rs5219 风险等位基因的参与者的血液胰岛素水平和胰岛素分泌减少有关。此外,多元逻辑回归分析显示,风险等位基因组易受酒精摄入对β细胞功能损害的影响(OR 1.450;95%CI 1.061-1.982)。此外,12 年的随访结果表明,酒精摄入与 KCNJ11 rs5219 风险等位基因的参与者的胰岛素分泌协同下降。我们的研究结果表明,KCNJ11 rs5219 风险等位基因与酒精摄入相结合可能是β细胞功能障碍的一个潜在危险因素。我们希望这一新发现能够有助于进一步了解在个体遗传背景的基础上,酒精摄入与 T2D 发展的关系。