Late Diagnosis of POMC Deficiency and In Vitro Evidence of Residual Translation From Allele With c.-11C>A Mutation

A. Anisimova, P. Rubtsov, K. A. Akulich, S. Dmitriev, E. Frolova, A. Tiulpakov
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引用次数: 12

Abstract

Context: Loss-of-function mutations in the POMC gene are associated with a syndrome with the characteristics of adrenal insufficiency, obesity, and red hair. We describe here a case of pro-opiomelanocortin (POMC) deficiency in which adrenal insufficiency was not treated until the fourth year of life. One of the disease-causative POMC mutations was characterized in vitro using a unique approach. Case Description: A boy presented in the first year of life with red hair, growth acceleration, moderate obesity, and recurrent cholestasis, which was followed by 2 episodes of hypoglycemia at the ages of 1.5 and 3 years. The diagnosis was suspected at the age of 3.6 years after documentation of undetectable levels of plasma adrenocorticotropic hormone and serum cortisol, after which replacement with hydrocortisone was initiated. Sequencing of the POMC gene revealed compound heterozygosity for c.-11C>A/p.W84X mutations. The p.W84X mutation is predicted to result in a marked truncation of preprohormone. Using a messenger RNA transfection approach followed by an in vitro translation assay, we could directly demonstrate that the transcript with c.-11C>A substitution is predominantly translated within a new open reading frame; however, translation of the POMC main reading frame is preserved, with translation efficiency being ∼17% of the wild-type transcript. Conclusions: The current report provides important information on the natural course of POMC deficiency. In vitro translation studies demonstrated residual translation of the main coding region from an allele with the c.-11C>A mutation, which at least partially explains a relatively late presentation of adrenal insufficiency in the patient.
POMC缺乏症的晚期诊断和c - 11c >A突变等位基因残留翻译的体外证据
背景:POMC基因的功能缺失突变与一种以肾上腺功能不全、肥胖和红发为特征的综合征相关。我们在这里描述的情况下,促阿片黑素皮质素(POMC)缺乏,其中肾上腺功能不全没有治疗,直到第四年的生活。一种致病的POMC突变在体外使用一种独特的方法进行了表征。病例描述:一名男孩在出生第一年出现红发、生长加速、中度肥胖和复发性胆汁淤积,随后在1.5岁和3岁时出现2次低血糖发作。在3.6岁时,在血浆促肾上腺皮质激素和血清皮质醇水平未检测到后,怀疑诊断,随后开始用氢化可的松替代。POMC基因测序显示c - 11c >A/p的复合杂合性。W84X突变。据预测,p.W84X突变会导致激素前体的显著截断。使用信使RNA转染方法和体外翻译实验,我们可以直接证明具有c - 11c > a替换的转录本主要在新的开放阅读框内翻译;然而,POMC主阅读框的翻译被保留下来,翻译效率为野生型转录物的17%。结论:本报告为POMC缺乏的自然过程提供了重要信息。体外翻译研究表明,c - 11c >A突变等位基因的主要编码区存在残留翻译,这至少部分解释了患者相对较晚出现肾上腺功能不全的原因。
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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