Diabetes Insipidus as an Early Clinical Indicator of Wolfram Syndrome Type 1: Evidence From a Symptom-Based Screening Approach.

IF 5.6 3区医学 Q2 ENDOCRINOLOGY & METABOLISM

Pediatric Diabetes Pub Date : 2025-10-02 eCollection Date: 2025-01-01 DOI:10.1155/pedi/8692152

Ozge Beyza Gundogdu Ogutlu, Atilla Cayır, Ayşe Sena Donmez, Serkan Bilge Koca, Oguzhan Yarali, Huseyin Demirbilek

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引用次数: 0

Abstract

Objective: Wolfram Syndrome Type 1 (WS1) is a rare neurodegenerative disorder characterized by diabetes insipidus (DI), diabetes mellitus (DM), optic atrophy (OA), and deafness (D) due to biallelic mutations in the WFS1 gene. As the cardinal symptoms of DI, polyuria and polydipsia, overlap with those of DM, DI might be underdiagnosed or delayed in the early stages of WS1. In the present study, we assessed whether DI could be an early sign of WS1 and analyzed genotype-phenotype correlations in a group of Turkish patients with Type 1 DM. Patients and Methods: We applied a polyuria/polydipsia questionnaire to 1278 children with Type 1 DM. Patients with suggestive symptoms of DI were further evaluated for other clinical features of WS1 and molecular genetic analysis of the WFS1 gene. Clinical, laboratory, and genetic characteristics of cases identified using questionnaires were compared with a historical case series of seven children with WS1 and previously published literature data. Results: Eighteen patients were considered to have a diagnosis of DI, thereby being eligible for genetic analysis of WFS1 variants. Of those, six had biallelic variations (four missense variants, one in-frame duplication, and three frameshift variants) in the WFS1 gene, and a diagnosis of WS1 was confirmed. The age of admission for DM was younger in the historical cases (5.1 ± 2.0 vs. 8.7 ± 3.4; p=0.04). There was no statistically significant difference between the ages for the diagnosis of WS1 (12.9 ± 5.0 vs. 9.6 ± 2.7; p=0.191), though the diagnostic delay from DM onset to WS1 diagnosis was significantly shorter in the screened group (median 1.8 vs. 6.9 years; p ≈ 0.015). Conclusion: Our findings suggest that DI may present before OA in WS1. Enriching the diagnosis of DI using a simple polyuria/polydipsia questionnaire may provide an earlier diagnosis of WS1 in patients followed with Type 1 DM. Screening and early genetic testing of these patients enhances the diagnosis, follow-up, and management strategies of patients with WS1.

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尿崩症作为Wolfram综合征1型的早期临床指标：来自症状筛选方法的证据

目的：Wolfram综合征1型（WS1）是一种罕见的神经退行性疾病，以尿崩症（DI）、糖尿病（DM）、视神经萎缩（OA）和耳聋(D)为特征，由WFS1基因双等位基因突变引起。由于DI的主要症状是多尿和多饮，与DM的症状重叠，因此DI可能在WS1的早期诊断不足或延迟。在本研究中，我们评估了DI是否可能是WS1的早期征兆，并分析了一组土耳其1型糖尿病患者的基因型-表型相关性。患者和方法：我们对1278名1型糖尿病儿童进行了多尿/多饮问卷调查。对有DI症状的患者进行了WS1的其他临床特征评估和WFS1基因的分子遗传分析。通过问卷调查确定的病例的临床、实验室和遗传特征与7名WS1患儿的历史病例系列和先前发表的文献数据进行比较。结果：18例患者被认为诊断为DI，因此有资格进行WFS1变异的遗传分析。其中，6例WFS1基因存在双等位变异（4例错义变异，1例帧内重复，3例移码变异），确诊为WS1。病史患者入院年龄较年轻（5.1±2.0∶8.7±3.4;p=0.04）。两组诊断WS1的年龄差异无统计学意义（12.9±5.0∶9.6±2.7;p=0.191），但筛查组从DM发病到WS1诊断的延迟时间明显缩短（中位1.8∶6.9年；p≈0.015）。结论：我们的研究结果表明，在WS1中，DI可能先于OA出现。通过简单的多尿/多饮问卷丰富对DI的诊断，可能为1型糖尿病患者早期诊断WS1提供帮助。对这些患者进行筛查和早期基因检测，可提高WS1患者的诊断、随访和管理策略。

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来源期刊

Pediatric Diabetes 医学-内分泌学与代谢

CiteScore

6.60

自引率

14.70%

发文量

141

审稿时长

4-8 weeks

期刊介绍： Pediatric Diabetes is a bi-monthly journal devoted to disseminating new knowledge relating to the epidemiology, etiology, pathogenesis, management, complications and prevention of diabetes in childhood and adolescence. The aim of the journal is to become the leading vehicle for international dissemination of research and practice relating to diabetes in youth. Papers are considered for publication based on the rigor of scientific approach, novelty, and importance for understanding mechanisms involved in the epidemiology and etiology of this disease, especially its molecular, biochemical and physiological aspects. Work relating to the clinical presentation, course, management and outcome of diabetes, including its physical and emotional sequelae, is considered. In vitro studies using animal or human tissues, whole animal and clinical studies in humans are also considered. The journal reviews full-length papers, preliminary communications with important new information, clinical reports, and reviews of major topics. Invited editorials, commentaries, and perspectives are a regular feature. The editors, based in the USA, Europe, and Australasia, maintain regular communications to assure rapid turnaround time of submitted manuscripts.