Phenotypic features, prevalence of KCNJ11‐MODY in Chinese patients with early‐onset diabetes and a literature review

医学 青少年成熟型糖尿病 队列 糖尿病 内科学 2型糖尿病 遗传学 内分泌学 生物
作者
Tianhao Ba,Qian Ren,Siqian Gong,Meng Li,Xiaoling Cai,Wei Liu,Yingying Luo,Simin Zhang,Rui Zhang,Lingli Zhou,Yu Zhu,X Zhang,Jing Chen,Jing Wu,Xianghai Zhou,Yufeng Li,Xirui Wang,Fang Wang,Liyong Zhong,Xueyao Han
出处
期刊:Clinical Endocrinology [Wiley]
卷期号:101 (5): 466-474
标识
DOI:10.1111/cen.15126
摘要

Abstract Objective Gain‐of‐function (GOF) variants of KCNJ11 cause neonate diabetes and maturity‐onset diabetes of the young ( KCNJ11 ‐MODY), while loss‐of‐function (LOF) variants lead to hyperinsulinemia hypoglycemia and subsequent diabetes. Given the limited research of KCNJ11 ‐MODY, we aimed to analyse its phenotypic features and prevalence in Chinese patients with early‐onset type 2 diabetes (EOD). Design, Patients and Measurements We performed next‐generation sequencing on 679 Chinese EOD patients to screen for KCNJ11 exons variants. Bioinformatics prediction and the American College of Medical Genetics and Genomics guidelines was used to determine the pathogenicity and diagnosed KCNJ11 ‐MODY. A literature review was conducted to investigate the phenotypic features of KCNJ11 ‐MODY. Results We identified six predicted deleterious rare variants in six EOD patients (0.88%). They were classified as uncertain significance (variant of uncertain significance [VUS]), but more common in this EOD cohort than a general Chinese population database, however, without significant difference (53/10,588, 0.50%) ( p = .268). Among 80 previously reported patients with KCNJ11 ‐MODY, 23.8% (19/80) carried 9 (32.1%) LOF variants, who had significantly older age at diagnosis, higher birthweight and higher fasting C‐peptide compared to patients with GOF variants. Many patients carrying VUS were not correctly diagnosed. Conclusions Some rare variants of KCNJ11 might contribute to the development of Chinese EOD, although available evidence has not enough power to support them as cause of KCNJ11 ‐MODY. The clinical features of LOF variants were different from GOF variants in KCNJ11 ‐MODY patients. It is necessary to evaluate the pathogenicity of VUS through function experiments.
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