Our Experiences and Learnings in Diagnosing MODY from Non-Institutional-Based Diabetes Care Clinics.

Indian Journal of Endocrinology and Metabolism Pub Date : 2024-09-01 Epub Date: 2024-11-08 DOI:10.4103/ijem.ijem_361_23

Arunkumar R Pande, Santosh Chaubey, Dinesh Kumar, Kumar P Chandra, Thenral Geetha, Akshita Sharma

{"title":"Our Experiences and Learnings in Diagnosing MODY from Non-Institutional-Based Diabetes Care Clinics.","authors":"Arunkumar R Pande, Santosh Chaubey, Dinesh Kumar, Kumar P Chandra, Thenral Geetha, Akshita Sharma","doi":"10.4103/ijem.ijem_361_23","DOIUrl":null,"url":null,"abstract":"Introduction: Maturity-onset diabetes of the young (MODY) is a rare group of disorders characterised by impaired functions or development of pancreatic islets and monogenic diabetes at a young age. Diagnosing MODY can be rewarding for both clinicians and patients as it can change the management from generic to targeted therapy.Methods: This study reports the retrospective analysis of data collected from four clinics between March 2016 and February 2023 from Lucknow, a city in northern India. Fifty-three individuals are suspected to be affected by MODY based on ISPAD guidelines. Following a detailed clinical evaluation, they were referred for genetic diagnostic testing.Results: The cohort consists of 19 females and 34 males with a mean age of diagnosis of 25.3 years and a body mass index of 22.3 Kg/m2. Genetic testing detected variants in 13/53 (~24.5%) individuals. Five cases had significant pathogenic/likely pathogenic variants, HNF1A gene in two [(p.Phe268LeufsTer74) (p.Arg200Gln)], one each in HNF4A (Arg311His), PDX1(p.Ala228GlyfsTer33), and a case with suggestive digenic variants in HNF1A gene (p.Arg200Gln) and HNF1B [(p.Leu13Met)]. Variants of uncertain significance (VUSs) with inconclusive evidence of pathogenicity were reported in eight patients, and five were considered to be clinically significant as they are lean young onset, sulfonylurea-responsive, and presented with diabetes without acanthosis nigricans and with high pretest probability. These individuals harboured variants in HNF1A (p.Thr425_Thr429delinsPro), HNF1B (p.Ser19Phe), CEL (p.Val681ArgfsTer6), ABCC8 (p.Ile872Met), and KCNJ11 (p.Arg221Cys) genes.Conclusion: We found a diagnostic yield of around 10% of pathogenic or likely pathogenic variants in individuals who were suspected to have MODY. As it is a field that is still evolving, we might consider starting with oral agents under close supervision in those individuals who have VUS; there are some proportions of individuals who might not have classical sulfonylurea-responsive genetic variants, but they might respond to it.","PeriodicalId":13353,"journal":{"name":"Indian Journal of Endocrinology and Metabolism","volume":"28 5","pages":"480-487"},"PeriodicalIF":0.0000,"publicationDate":"2024-09-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11642506/pdf/","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Indian Journal of Endocrinology and Metabolism","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.4103/ijem.ijem_361_23","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"2024/11/8 0:00:00","PubModel":"Epub","JCR":"","JCRName":"","Score":null,"Total":0}

引用次数: 0

Abstract

Introduction: Maturity-onset diabetes of the young (MODY) is a rare group of disorders characterised by impaired functions or development of pancreatic islets and monogenic diabetes at a young age. Diagnosing MODY can be rewarding for both clinicians and patients as it can change the management from generic to targeted therapy.

Methods: This study reports the retrospective analysis of data collected from four clinics between March 2016 and February 2023 from Lucknow, a city in northern India. Fifty-three individuals are suspected to be affected by MODY based on ISPAD guidelines. Following a detailed clinical evaluation, they were referred for genetic diagnostic testing.

Results: The cohort consists of 19 females and 34 males with a mean age of diagnosis of 25.3 years and a body mass index of 22.3 Kg/m². Genetic testing detected variants in 13/53 (~24.5%) individuals. Five cases had significant pathogenic/likely pathogenic variants, HNF1A gene in two [(p.Phe268LeufsTer74) (p.Arg200Gln)], one each in HNF4A (Arg311His), PDX1(p.Ala228GlyfsTer33), and a case with suggestive digenic variants in HNF1A gene (p.Arg200Gln) and HNF1B [(p.Leu13Met)]. Variants of uncertain significance (VUSs) with inconclusive evidence of pathogenicity were reported in eight patients, and five were considered to be clinically significant as they are lean young onset, sulfonylurea-responsive, and presented with diabetes without acanthosis nigricans and with high pretest probability. These individuals harboured variants in HNF1A (p.Thr425_Thr429delinsPro), HNF1B (p.Ser19Phe), CEL (p.Val681ArgfsTer6), ABCC8 (p.Ile872Met), and KCNJ11 (p.Arg221Cys) genes.

Conclusion: We found a diagnostic yield of around 10% of pathogenic or likely pathogenic variants in individuals who were suspected to have MODY. As it is a field that is still evolving, we might consider starting with oral agents under close supervision in those individuals who have VUS; there are some proportions of individuals who might not have classical sulfonylurea-responsive genetic variants, but they might respond to it.

查看原文

微信好友朋友圈 QQ好友复制链接

本刊更多论文

我们从非机构糖尿病护理诊所诊断 MODY 的经验和教训。

简介年轻成熟型糖尿病（MODY）是一组罕见的疾病，其特征是胰岛功能或发育受损，并在年轻时出现单基因糖尿病。诊断出 MODY 对临床医生和患者都有好处，因为它可以将治疗方法从普通疗法转变为针对性疗法：本研究对 2016 年 3 月至 2023 年 2 月期间从印度北部城市勒克瑙的四家诊所收集的数据进行了回顾性分析。根据 ISPAD 指南，53 人被怀疑患有 MODY。经过详细的临床评估后，他们被转诊接受基因诊断检测：结果：队列中有 19 名女性和 34 名男性，平均诊断年龄为 25.3 岁，体重指数为 22.3 Kg/m2。基因检测在 13/53 人（约占 24.5%）中发现了变异。五个病例有明显的致病/可能致病变异，其中两个是 HNF1A 基因[(p.Phe268LeufsTer74) (p.Arg200Gln)]，HNF4A (Arg311His)、PDX1(p.Ala228GlyfsTer33)各一个，还有一个病例有提示性的 HNF1A 基因（p.Arg200Gln）和 HNF1B [(p.Leu13Met)]二基因变异。有 8 名患者报告了致病性证据不确定的意义不明变异（VUS），其中 5 名患者被认为具有临床意义，因为他们都是年轻的瘦弱患者，对磺脲类药物有反应，并且表现为无黑棘皮病的糖尿病，而且预试概率很高。这些人携带 HNF1A（p.Thr425_Thr429delinsPro）、HNF1B（p.Ser19Phe）、CEL（p.Val681ArgfsTer6）、ABCC8（p.Ile872Met）和 KCNJ11（p.Arg221Cys）基因变异：我们发现，在疑似患有 MODY 的个体中，致病或可能致病变异的诊断率约为 10%。由于这一领域仍在不断发展，我们可以考虑在密切监督下，从口服药物开始，对那些有 VUS 的人进行治疗；有一部分人可能没有经典的磺脲类药物反应基因变异，但他们可能会对磺脲类药物产生反应。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

求助全文

约1分钟内获得全文去求助

来源期刊

Indian Journal of Endocrinology and Metabolism Medicine-Endocrinology, Diabetes and Metabolism

CiteScore

2.10

自引率

0.00%

发文量

期刊介绍： The Indian Journal of Endocrinology and Metabolism (IJEM) aims to function as the global face of Indian endocrinology research. It aims to act as a bridge between global and national advances in this field. The journal publishes thought-provoking editorials, comprehensive reviews, cutting-edge original research, focused brief communications and insightful letters to editor. The journal encourages authors to submit articles addressing aspects of science related to Endocrinology and Metabolism in particular Diabetology. Articles related to Clinical and Tropical endocrinology are especially encouraged. Sub-topic based Supplements are published regularly. This allows the journal to highlight issues relevant to Endocrine practitioners working in India as well as other countries. IJEM is free access in the true sense of the word, (it charges neither authors nor readers) and this enhances its global appeal.