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基因与酒精摄入之间的相互作用会影响胰岛素敏感性和β细胞功能。

Interactions of genes with alcohol consumption affect insulin sensitivity and beta cell function.

作者信息

Fu Qi, Dai Hao, Shen Sipeng, He Yunqiang, Zheng Shuai, Jiang Hemin, Gu Pan, Sun Min, Zhu Xiaowei, Xu Kuanfeng, Yang Tao

机构信息

Department of Endocrinology and Metabolism, the First Affiliated Hospital of Nanjing Medical University, Nanjing, China.

Department of Biostatistics, Center for Global Health, School of Public Health, Nanjing Medical University, Nanjing, China.

出版信息

Diabetologia. 2025 Jan;68(1):116-127. doi: 10.1007/s00125-024-06291-5. Epub 2024 Oct 19.

Abstract

AIMS/HYPOTHESIS: Alcohol consumption has complex effects on diabetes and metabolic disease, but there is widespread heterogeneity within populations and the specific reasons are unclear. Genetic factors may play a role and warrant exploration. The aim of this study was to elucidate genetic variants modulating the impact of alcohol consumption on insulin sensitivity and pancreatic beta cell function within populations presenting normal glucose tolerance (NGT).

METHODS

We recruited 4194 volunteers in Nanjing, 854 in Jurong and an additional 5833 in Nanjing for Discovery cohorts 1 and 2 and a Validation cohort, respectively. We performed an OGTT on all participants, establishing a stringent NGT group, and then assessed insulin sensitivity and beta cell function. Alcohol consumption was categorised as abstinent, light-to-moderate (<210 g per week) or heavy (≥210 g per week). After excluding ineligible individuals, an exploratory genome-wide association study identified potential variants interacting with alcohol consumption in 1862 NGT individuals. These findings were validated in an additional cohort of 2169 NGT individuals. Cox proportional hazard regression was further employed to evaluate the effect of the interaction between the potential variants and alcohol consumption on the risk of type 2 diabetes within the UK Biobank cohort.

RESULTS

A significant correlation was observed between drinking levels and insulin sensitivity, accompanied by a consequent inverse relationship with insulin resistance and beta cell insulin secretion after adjusting for confounding factors in NGT individuals. However, no significant associations were noted in the disposition indexes. The interaction of variant rs56221195 with alcohol intake exhibited a pronounced effect on the liver insulin resistance index (LIRI) in the discovery set, corroborated in the validation set (combined p=1.32 × 10). Alcohol consumption did not significantly affect LIRI in rs56221195 wild-type (TT) carriers, but a strong negative association emerged in heterozygous (TA) and homozygous (AA) individuals. The rs56221195 variant also significantly interacts with alcohol consumption, influencing the total insulin secretion index INSR120 (the ratio of the AUC of insulin to glucose from 0 to 120 min) (p=2.06 × 10) but not disposition index. In the UK Biobank, we found a significant interaction between rs56221195 and alcohol consumption, which was linked to the risk of type 2 diabetes (HR 0.897, p=0.008).

CONCLUSIONS/INTERPRETATION: Our findings reveal the effects of the interaction of alcohol and rs56221195 on hepatic insulin sensitivity in NGT individuals. It is imperative to weigh potential benefits and detriments thoughtfully when considering alcohol consumption across diverse genetic backgrounds.

摘要

目的/假设:饮酒对糖尿病和代谢性疾病具有复杂影响,但人群中存在广泛的异质性,具体原因尚不清楚。遗传因素可能起作用,值得探索。本研究的目的是阐明在糖耐量正常(NGT)人群中调节饮酒对胰岛素敏感性和胰岛β细胞功能影响的基因变异。

方法

我们分别在南京招募了4194名志愿者、在句容招募了854名志愿者,并在南京另外招募了5833名志愿者作为发现队列1、发现队列2和验证队列。我们对所有参与者进行了口服葡萄糖耐量试验(OGTT),建立了一个严格的NGT组,然后评估胰岛素敏感性和β细胞功能。饮酒情况分为戒酒、轻度至中度(每周<210克)或重度(每周≥210克)。在排除不符合条件的个体后,一项探索性全基因组关联研究在1862名NGT个体中确定了与饮酒相互作用的潜在变异。这些发现在另外2169名NGT个体的队列中得到了验证。进一步采用Cox比例风险回归来评估潜在变异与饮酒之间的相互作用对英国生物银行队列中2型糖尿病风险的影响。

结果

在NGT个体中,调整混杂因素后,观察到饮酒水平与胰岛素敏感性之间存在显著相关性,随之与胰岛素抵抗和β细胞胰岛素分泌呈负相关。然而,在处置指数中未发现显著关联。变异rs56221195与酒精摄入量的相互作用在发现集中对肝脏胰岛素抵抗指数(LIRI)有显著影响,在验证集中得到证实(合并p=1.32×10)。在rs56221195野生型(TT)携带者中,饮酒对LIRI没有显著影响,但在杂合子(TA)和纯合子(AA)个体中出现了强烈的负相关。rs56221195变异也与酒精消费显著相互作用,影响总胰岛素分泌指数INSR120(0至120分钟胰岛素与葡萄糖曲线下面积的比值)(p=2.06×10),但不影响处置指数。在英国生物银行中,我们发现rs56221195与酒精消费之间存在显著相互作用,这与2型糖尿病风险相关(风险比0.897,p=0.008)。

结论/解读:我们的研究结果揭示了酒精与rs56221195相互作用对NGT个体肝脏胰岛素敏感性的影响。在考虑不同遗传背景下的饮酒问题时,必须谨慎权衡潜在的益处和危害。

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