Diverse Phenotypes of Mitochondrial Disease With Varying Levels of Heteroplasmy.

JCEM case reports Pub Date : 2025-03-26 eCollection Date: 2025-04-01 DOI:10.1210/jcemcr/luaf020

Rebecca John, Aaron Chapla, Geeta Chacko, Sangeetha Yoganathan, Maya Mary Thomas, Nihal Thomas

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Abstract

Mitochondrial diseases have a wide spectrum of clinical presentations. Heteroplasmy, the presence of wild type and mutated mitochondrial deoxyribonucleic acid (DNA) in a single cell, is typical of mitochondrial disorders. It can show varying levels between cells of the same tissue, between organs in a single individual as well as between members of the same family. We describe below a woman who presented to us for management of pancreatic diabetes. Her daughter had a history of recurrent bouts of myopathy; evaluation was suggestive of having a mitochondrial etiology. Subsequently, mitochondrial genetic testing revealed positivity for m.3243A>G variant with a heteroplasmy of 45% in the blood in the daughter and 15% in the proband. We highlight how differences in the heteroplasmy and threshold levels among members of the same family resulted in a variable spectrum of clinical disease. Family screening of members identified with mitochondrial disease is of utmost significance to ensure early diagnosis and therapy.

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线粒体疾病的不同表型与不同水平的异质性。

线粒体疾病具有广泛的临床表现。异质性，即在单个细胞中存在野生型和突变的线粒体脱氧核糖核酸（DNA），是线粒体疾病的典型特征。它可以显示同一组织的不同细胞之间、同一个体的不同器官之间以及同一家族成员之间的不同水平。我们在下面描述一位向我们提出治疗胰腺糖尿病的妇女。她的女儿有反复发作的肌病病史；评估提示有线粒体病因。随后，线粒体基因检测显示m.3243A >g变异阳性，女儿血液异质性为45%，先证血异质性为15%。我们强调异质性和阈值水平在同一家族成员之间的差异如何导致临床疾病的不同谱。对患有线粒体疾病的成员进行家庭筛查对于确保早期诊断和治疗至关重要。

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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JCEM case reports

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