日本年轻起病型糖尿病样糖尿病患者的靶向基因panel 分析:ABCC8 和胰岛素抵抗基因失活变异的作用。
Targeted gene panel analysis of Japanese patients with maturity-onset diabetes of the young-like diabetes mellitus: Roles of inactivating variants in the ABCC8 and insulin resistance genes.
机构信息
Division of Pediatric Endocrinology and Metabolism, Children's Medical Center, Osaka City General Hospital, Osaka, Japan.
Department of Genetic Medicine, Osaka City General Hospital, Osaka, Japan.
出版信息
J Diabetes Investig. 2023 Mar;14(3):387-403. doi: 10.1111/jdi.13957. Epub 2022 Dec 12.
AIMS/INTRODUCTION: To investigate the genetic background of Japanese patients with suspected maturity-onset diabetes of the young (MODY).
MATERIALS AND METHODS
On 340 proband patients referred from across Japan, genomic variants were analyzed using a targeted multigene panel analysis combined with the multiplex ligation probe amplification (MLPA) analysis, mitochondrial m.3243A > G analysis and methylation-specific polymerase chain reaction of the imprinted 6q24 locus. Pathogenic/likely pathogenic variants were listed according to the 2015 American College of Medical Genetics and Genomics and the Association for Molecular Pathology criteria. Additionally, variants with a population frequency <0.001 and Combined Annotation Dependent Depletion score >20 (CS >20) were listed as rare variants of uncertain significance-CS >20.
RESULTS
A total of 157 pathogenic/likely pathogenic variants and 44 rare variants of uncertain significance-CS >20 were identified. In the pathogenic/likely pathogenic variants, alterations in the GCK gene were the most common (82, 52.2%) followed by HNF1A (29, 18.5%), HNF4A (13, 8.3%) and HNF1B (13, 8.3%). One patient was a 29.5% mosaic with a truncating INSR variant. In the rare variants of uncertain significance-CS >20, 20 (45.5%) were in the genes coding for the adenosine triphosphate-sensitive potassium channel, KCNJ11 or ABCC8, and four were in the genes of the insulin-signaling pathway, INSR and PIK3R1. Four variants in ABCC8 were previously reported in patients with congenital hyperinsulinism, suggesting the inactivating nature of these variants, and at least two of our patients had a history of congenital hyperinsulinism evolving into diabetes. In two patients with INSR or PIK3R1 variants, insulin resistance was evident at diagnosis.
CONCLUSIONS
Causative genomic variants could be identified in at least 46.2% of clinically suspected MODY patients. ABCC8-MODY with inactivating variants could represent a distinct category of MODY. Genes of insulin resistance should be included in the sequencing panel for MODY.
目的/引言:研究疑似青少年起病成年型糖尿病(MODY)日本患者的遗传背景。
材料与方法
对来自日本各地的 340 名先证者患者,采用靶向多基因panel 分析结合多重连接探针扩增(MLPA)分析、线粒体 m.3243A>G 分析和印迹 6q24 基因座的甲基化特异性聚合酶链反应,对基因组变异进行分析。根据 2015 年美国医学遗传学与基因组学学会和分子病理学协会的标准,列出致病性/可能致病性变异。此外,将群体频率<0.001 且综合注释依赖耗竭评分>20(CS>20)的变异列为 CS>20 的罕见意义不明变异。
结果
共发现 157 种致病性/可能致病性变异和 44 种 CS>20 的罕见意义不明变异。在致病性/可能致病性变异中,GCK 基因突变最为常见(82 例,52.2%),其次是 HNF1A(29 例,18.5%)、HNF4A(13 例,8.3%)和 HNF1B(13 例,8.3%)。1 例患者为截断 INSR 变异的 29.5%嵌合体。在 CS>20 的罕见意义不明变异中,20 种(45.5%)为编码三磷酸腺苷敏感钾通道的基因 KCNJ11 或 ABCC8 的变异,4 种为胰岛素信号通路的基因 INSR 和 PIK3R1 的变异。ABCC8 的 4 种变异之前在先天性高胰岛素血症患者中报道过,提示这些变异具有失活性质,我们至少有 2 例患者有先天性高胰岛素血症进展为糖尿病的病史。在 2 例 INSR 或 PIK3R1 变异患者中,诊断时存在胰岛素抵抗。
结论
至少 46.2%的临床疑似 MODY 患者可确定致病的基因组变异。具有失活变异的 ABCC8-MODY 可能代表 MODY 的一个独特类别。胰岛素抵抗相关基因应纳入 MODY 测序panel。
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