Rare MTNR1B variants causing diminished MT2 signalling associate with elevated HbA1c levels but not with type 2 diabetes

IF 8.4 1区医学 Q1 ENDOCRINOLOGY & METABOLISM

Diabetologia Pub Date : 2025-03-10 DOI:10.1007/s00125-025-06381-y

Kimmie V. Sørensen, Johanne M. Justesen, Lars Ängquist, Jette Bork-Jensen, Bolette Hartmann, Niklas R. Jørgensen, Jørgen Rungby, Henrik T. Sørensen, Allan Vaag, Jens S. Nielsen, Jens J. Holst, Oluf Pedersen, Allan Linneberg, Torben Hansen, Niels Grarup

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引用次数: 0

Abstract

Aims/hypothesis

An intronic variant (rs10830963) in MTNR1B (encoding the melatonin receptor type 2 [MT2]) has been shown to strongly associate with impaired glucose regulation and elevated type 2 diabetes prevalence. However, MTNR1B missense variants have shown conflicting results on type 2 diabetes. Thus, we aimed to gain further insights into the impact of MTNR1B coding variants on type 2 diabetes prevalence and related phenotypes.

Methods

We conducted a cross-sectional study, performing MTNR1B variant burden testing of glycaemic phenotypes (N=248,454, without diabetes), other cardiometabolic phenotypes (N=330,453) and type 2 diabetes prevalence (case–control study; N=263,739) in the UK Biobank. Similar burden testing with glycaemic phenotypes was performed in Danish Inter99 participants without diabetes (N=5711), and type 2 diabetes prevalence (DD2 cohort serving as cases [N=2930] and Inter99 serving as controls [N=4243]). Finally, we evaluated the effects of MTNR1B variants on the melatonin-induced glucose regulation response in a recall-by-genotype study of individuals without diabetes.

Results

In the UK Biobank, MTNR1B variants were not associated with cardiometabolic phenotypes, including type 2 diabetes prevalence, except that carriers of missense MTNR1B variants causing impaired MT2 signalling exhibited higher HbA_1c levels compared with non-carriers (effect size, β, 0.087 SD [95% CI 0.039, 0.135]). Similarly, no significant associations were observed with phenotypes associated with glycaemic phenotypes in the Inter99 population. However, carriers of variants impairing MT2 signalling demonstrated a nominally significant lower glucose-stimulated insulin response (β −0.47 SD [95% CI −0.82, −0.11]). A reduced insulin response was also observed in carriers of variants impairing MT2 signalling (β −476.0 [95% CI −928.6, −24.4]) or the rs10830963 variant (β −390.8 [95% CI −740.1, −41.6]) compared with non-carriers after melatonin treatment.

Conclusions/interpretation

The higher type 2 diabetes prevalence previously observed in carriers of missense MTNR1B variants causing impairment in MT2 signalling was not replicated in the UK Biobank, yet carriers had elevated HbA_1c levels.

Data availability

Data (Inter99 cohort and recall-by-genotype study) are available on reasonable request from the corresponding author. Requests for DD2 data are through the application form at https://dd2.dk/forskning/ansoeg-om-data. Access to UK Biobank data can be requested through the UK Biobank website (https://www.ukbiobank.ac.uk/enable-your-research).

Graphical Abstract

查看原文本刊更多论文

目的/假说MTNR1B（编码 2 型褪黑激素受体 [MT2]）的一个内含子变异（rs10830963）已被证明与葡萄糖调节功能受损和 2 型糖尿病患病率升高密切相关。然而，MTNR1B 错义变异对 2 型糖尿病的影响结果并不一致。因此，我们旨在进一步了解 MTNR1B 编码变异对 2 型糖尿病患病率和相关表型的影响。方法我们在英国生物库中进行了一项横断面研究，对血糖表型（N=248,454，无糖尿病）、其他心脏代谢表型（N=330,453）和 2 型糖尿病患病率（病例对照研究；N=263,739）进行了 MTNR1B 变异负担测试。在丹麦 Inter99 无糖尿病参与者（N=5711）和 2 型糖尿病患病率（DD2 队列作为病例[N=2930]，Inter99 作为对照[N=4243]）中进行了类似的糖代谢表型负担测试。最后，我们在对无糖尿病个体进行的逐基因型回忆研究中评估了 MTNR1B 变体对褪黑激素诱导的葡萄糖调节反应的影响。结果在英国生物库中，MTNR1B 变体与心脏代谢表型（包括 2 型糖尿病患病率）无关，但导致 MT2 信号受损的错义 MTNR1B 变体携带者的 HbA1c 水平高于非携带者（效应大小，β，0.087 SD [95% CI 0.039, 0.135]）。同样，在 Inter99 群体中，也没有观察到与血糖表型相关的表型有明显的关联。然而，MT2 信号受损变异携带者的葡萄糖刺激胰岛素反应明显降低（β -0.47 SD [95% CI -0.82，-0.11]）。在褪黑激素治疗后，与非携带者相比，MT2 信号受损变异携带者（β -476.0 [95% CI -928.6, -24.4]）或 rs10830963 变异携带者（β -390.8 [95% CI -740.1, -41.6]）的胰岛素反应也有所降低。结论/解释之前在英国生物库中观察到的导致MT2信号受损的错义MTNR1B变异携带者中较高的2型糖尿病患病率并未得到证实，但携带者的HbA1c水平升高。如需 DD2 数据，请通过 https://dd2.dk/forskning/ansoeg-om-data 上的申请表提出申请。可通过英国生物库网站（https://www.ukbiobank.ac.uk/enable-your-research）申请访问英国生物库数据。图表摘要

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Diabetologia 医学-内分泌学与代谢

CiteScore

18.10

自引率

2.40%

发文量

193

审稿时长

1 months

期刊介绍： Diabetologia, the authoritative journal dedicated to diabetes research, holds high visibility through society membership, libraries, and social media. As the official journal of the European Association for the Study of Diabetes, it is ranked in the top quartile of the 2019 JCR Impact Factors in the Endocrinology & Metabolism category. The journal boasts dedicated and expert editorial teams committed to supporting authors throughout the peer review process.