Identification of heterozygous mutations of ABCC8 gene responsible for maturity-onset diabetes of the young with exome sequencing.

IF 3.1 3区医学 Q2 ENDOCRINOLOGY & METABOLISM

Acta Diabetologica Pub Date : 2024-11-18 DOI:10.1007/s00592-024-02410-1

Yanxia Liu, Shuxin Ren, Chaofeng Zhu, Sufang Chen, Huijuan Zhang, Juan Zhang, Jianhua Li, Yanyan Jiang

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引用次数: 0

Abstract

Background: Although the MODY12 subtype, caused by ABCC8 mutations, is rare, it is highly sensitive to sulfonylureas. The identification of ABCC8 mutations in patients clinically diagnosed with MODY has the ability to contribute to the precise management of diabetes.

Methods: Genetic analysis of two families with MODY were conducted using whole-exome sequencing (WES) and Sanger sequencing. The spatial structures of the mutant proteins were constructed using MODELLER and PyMOL software to provide further evidence of pathogenicity.

Results: The heterozygous missense mutations V357I and R1393H in ABCC8 were found in probands of two unrelated MODY pedigrees, which co-segregated with the hyperglycemic phenotypes in these two pedigrees. Detection of the V357I mutation enabled the proband of family A to successfully transfer from insulin to sulfonylurea (SU). After 3 months of follow-up for the SU trial, the HbA1c level of proband A improved from 12.4% at the initial diagnosis to 7.20%. Proband B was treated with insulin because of pregnancy and poor islet function. In silico analysis indicated that the R1393H mutation resulted in a longer hydrogen bond distance to L1389 and cleavage of carbon-hydrogen bonds to V1395, A1390, and L1389.

Conclusions: We have described two pathogenic missense mutations in ABCC8 in Chinese families with MODY. Our findings support the heterogeneity in the clinical features of MODY12 caused by ABCC8 mutations.

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利用外显子组测序鉴定导致青年成熟型糖尿病的 ABCC8 基因杂合突变。

背景：由ABCC8突变引起的MODY12亚型虽然罕见，但对磺脲类药物高度敏感。在临床诊断为 MODY 的患者中鉴定 ABCC8 基因突变有助于糖尿病的精确治疗：方法：利用全外显子组测序（WES）和桑格测序对两个患有 MODY 的家族进行了基因分析。方法：利用全外显子组测序（WES）和桑格测序对两个MODY家族进行了遗传分析，并使用MODELLER和PyMOL软件构建了突变蛋白的空间结构，为致病性提供了进一步的证据：结果：在两个无血缘关系的MODY血统中发现了ABCC8中的杂合错义突变V357I和R1393H，这两个突变与这两个血统中的高血糖表型共存。V357I 基因突变的发现使 A 家系的患者成功地从胰岛素转为磺脲类药物（SU）。经过 3 个月的 SU 试验随访，原发性 A 的 HbA1c 水平从最初诊断时的 12.4% 降至 7.20%。由于怀孕和胰岛功能不佳，原患者 B 接受了胰岛素治疗。硅学分析表明，R1393H 突变导致与 L1389 的氢键距离变长，与 V1395、A1390 和 L1389 的碳氢键断裂：我们描述了中国 MODY 家族中 ABCC8 的两个致病性错义突变。我们的研究结果支持 ABCC8 突变导致的 MODY12 临床特征的异质性。

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

Acta Diabetologica 医学-内分泌学与代谢

CiteScore

7.30

自引率

2.60%

发文量

180

审稿时长

2 months

期刊介绍： Acta Diabetologica is a journal that publishes reports of experimental and clinical research on diabetes mellitus and related metabolic diseases. Original contributions on biochemical, physiological, pathophysiological and clinical aspects of research on diabetes and metabolic diseases are welcome. Reports are published in the form of original articles, short communications and letters to the editor. Invited reviews and editorials are also published. A Methodology forum, which publishes contributions on methodological aspects of diabetes in vivo and in vitro, is also available. The Editor-in-chief will be pleased to consider articles describing new techniques (e.g., new transplantation methods, metabolic models), of innovative importance in the field of diabetes/metabolism. Finally, workshop reports are also welcome in Acta Diabetologica.