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Assessment of MTNR1B Type 2 Diabetes Genetic Risk Modification by Shift Work and Morningness-Eveningness Preference in the UK Biobank

机译:评估MTNR1B 2型糖尿病遗传风险修改的换档工作和晨夜偏好于英国BIOBANK

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摘要

Night shift work, behavioral rhythms, and the common MTNR1B risk single nucleotide polymorphism (SNP), rs10830963, associate with type 2 diabetes; however, whether they exert joint effects to exacerbate type 2 diabetes risk is unknown. Among employed participants of European ancestry in the UK Biobank (N = 189,488), we aimed to test the cross-sectional independent associations and joint interaction effects of these risk factors on odds of type 2 diabetes (n = 5,042 cases) and HbA1c levels (n = 175,156). Current shift work, definite morning or evening preference, and MTNR1B rs10830963 risk allele associated with type 2 diabetes and HbA1c levels. The effect of rs10830963 was not modified by shift work schedules. While marginal evidence of interaction between self-reported morningness-eveningness preference and rs10830963 on risk of type 2 diabetes was seen, this interaction did not persist when analysis was expanded to include all participants regardless of employment status and when accelerometer-derived sleep midpoint was used as an objective measure of morningness-eveningness preference. Our findings suggest that MTNR1B risk allele carriers who carry out shift work or have more extreme morningness-eveningness preference may not have enhanced risk of type 2 diabetes.
机译:夜班工作,行为节律和常见的MTNR1B风险单核苷酸多态性(SNP),RS10830963,与2型糖尿病患者;但是,它们是否向加剧2型糖尿病风险发挥关节效应是未知的。在英国Biobank(N = 189,488)的欧洲祖先的参与者中,我们旨在测试这些危险因素的横断面独立关联和联合相互作用对2型糖尿病的几率(n = 5,042例)和HBA1C水平( n = 175,156)。当前班次工作,明确的早晨或晚间偏好,以及MTNR1B RS10830963风险等位基因与2型糖尿病和HBA1C水平相关。换档工作时间表没有修改RS10830963的效果。虽然在自我报告的辣妹 - 晚上偏好与患有2型糖尿病风险的互动的边缘证据,但在扩展分析以包括所有参与者的情况下,这种相互作用不存在,而不管就业状况以及使用加速度计衍生的睡眠中点作为晨天晚上偏好的客观衡量标准。我们的研究结果表明,MTNR1B风险等位基因载流子运行班次或具有更极端的晨夜偏好可能没有增强2型糖尿病的风险。

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