一种新的葡萄糖激酶突变家族成员的基因型-表型差异：对GCK-MODY及其与胰岛素抵抗的相互作用的见解

IF 7.5 1区医学 Q1 ENDOCRINOLOGY & METABOLISM

Diabetes Pub Date : 2025-09-25 DOI:10.2337/db24-1036

Shuhui Ji, Hua Shu, Hongqiang Zhao, Hongwei Jiang, Yuanyuan Ye, Xuan Liu, Shanshan Chen, Ying Yang, Wenli Feng, Jingting Qiao, Jinyang Zhen, Xiong Yang, Ziyue Zhang, Yu Fan, Yadi Huang, Qing He, Minxian Wang, Kunling Wang, Ming Liu

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引用次数: 0

摘要

葡萄糖激酶（GCK）基因的杂合失活突变导致年轻人的成熟型糖尿病（GCK- mody）。我们在两个表现出截然不同的糖尿病表型的家族成员中发现了GCK基因（c.77A>；T, p.Q26L）的一个不确定意义的新变体。为了探索GCK-Q26L突变的致糖尿病潜力，研究导致不同表型的单基因和多基因因素，我们对3名家族成员进行了全外显子组测序和多基因风险评分（PRS）评估。我们发现先证从她的父亲（患有轻度、稳定的高血糖）遗传了GCK-Q26L突变，但表现出更严重的糖尿病症状，包括多饮、多尿、体重减轻、酮症和明显的血脂异常。遗传分析将先证者的严重表型与她的胰岛素抵抗（IR）和2型糖尿病的高PRS联系起来。表达GCK-Q26L的敲入小鼠模型出现轻度高血糖、糖耐量受损、血清胰岛素降低和葡萄糖刺激胰岛素分泌受损。dorzagliatin和利拉鲁肽均能改善突变小鼠的葡萄糖耐量和胰岛素分泌。本研究表明GCK-Q26L是一种致病性GCK-MODY突变，其相关表型受IR和2型糖尿病PRS的影响。本研究旨在探讨一种新型GCK变异c.77A>；T, p.Q26L，在糖尿病表型有显著差异的两个家族成员中发现。我们旨在了解GCK-Q26L在葡萄糖代谢中的作用，并探讨遗传背景（包括胰岛素抵抗和2型糖尿病的多基因风险评分）是否与糖尿病表现有关。我们发现GCK-Q26L是导致GCK-MODY的致病突变，其严重程度由胰岛素抵抗和2型糖尿病的多基因风险评分调节。这些发现不仅扩大了GCK-MODY引起突变的列表，而且强调了多基因背景在单基因糖尿病的临床表现和管理中的重要性。

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Genotype-Phenotype Discrepancies in Family Members With a Novel Glucokinase Mutation: Insights Into GCK-MODY and Its Interplay With Insulin Resistance

Heterozygous inactivating mutations in the glucokinase (GCK) gene cause maturity-onset diabetes of the young (GCK-MODY). We identified a novel variant of uncertain significance in the GCK gene (c.77A>T, p.Q26L) in two family members exhibiting contrasting diabetic phenotypes. To explore the diabetogenic potential of the GCK-Q26L mutation and investigate the mono- and polygenetic factors contributing to different phenotypes, whole-exome sequencing and polygenic risk score (PRS) assessments were conducted on three family members. We found that the proband inherited the GCK-Q26L mutation from her father (who had mild, stable hyperglycemia) but exhibited more severe diabetic symptoms, including polydipsia, polyuria, weight loss, ketosis, and significant dyslipidemia. Genetic analysis linked the proband’s severe phenotypes to her high PRS for insulin resistance (IR) and type 2 diabetes. A global knock-in mouse model expressing GCK-Q26L presented mild hyperglycemia, impaired glucose tolerance, reduced serum insulin, and impaired glucose-stimulated insulin secretion. Both dorzagliatin and liraglutide improved glucose tolerance and insulin secretion in mutant mice. This study demonstrates that GCK-Q26L is a pathogenic GCK-MODY mutation, and its associated phenotypes are influenced by PRS for IR and type 2 diabetes. Article Highlights This study was undertaken to investigate the diabetogenic potential of a novel GCK variant, c.77A>T, p.Q26L, found in two family members with marked differences in diabetic phenotypes. We aimed to understand the role of GCK-Q26L in glucose metabolism and to explore whether genetic backgrounds, including polygenic risk score for insulin resistance and type 2 diabetes, contribute to diabetes manifestations. We found that GCK-Q26L is a pathogenic mutation leading to GCK-MODY, with severity modulated by polygenic risk score for insulin resistance and type 2 diabetes. These findings not only expand the list of GCK-MODY causing mutations but also highlight the importance of polygenic backgrounds in the clinical presentation and management of monogenic diabetes.

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来源期刊

Diabetes 医学-内分泌学与代谢

CiteScore

12.50

自引率

2.60%

发文量

1968

审稿时长

1 months

期刊介绍： Diabetes is a scientific journal that publishes original research exploring the physiological and pathophysiological aspects of diabetes mellitus. We encourage submissions of manuscripts pertaining to laboratory, animal, or human research, covering a wide range of topics. Our primary focus is on investigative reports investigating various aspects such as the development and progression of diabetes, along with its associated complications. We also welcome studies delving into normal and pathological pancreatic islet function and intermediary metabolism, as well as exploring the mechanisms of drug and hormone action from a pharmacological perspective. Additionally, we encourage submissions that delve into the biochemical and molecular aspects of both normal and abnormal biological processes. However, it is important to note that we do not publish studies relating to diabetes education or the application of accepted therapeutic and diagnostic approaches to patients with diabetes mellitus. Our aim is to provide a platform for research that contributes to advancing our understanding of the underlying mechanisms and processes of diabetes.