SCO1 突变导致的 COX 缺乏症的内分泌特征与癫痫性脑病：病例系列及文献综述

Endocrinological features and epileptic encephalopathy in COX deficiency due to SCO1 mutations: case series and review of literature.

作者信息

Barbato Alessandro, Gori Giulia, Sacchini Michele, Pochiero Francesca, Bargiacchi Sara, Traficante Giovanna, Palazzo Viviana, Tiberi Lucia, Bianchini Claudia, Mei Davide, Parrini Elena, Pisano Tiziana, Procopio Elena, Guerrini Renzo, Peron Angela, Stagi Stefano

机构信息

Auxo-endocrinology Unit, Meyer Children's Hospital IRCCS, Florence, Italy.

Department of Health Sciences, University of Florence, Florence, Italy.

出版信息

Endocr Connect. 2024 Sep 28;13(10). doi: 10.1530/EC-24-0221. Print 2024 Oct 1.

DOI:10.1530/EC-24-0221

PMID:39214134

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11466244/

Abstract

CONTEXT

Cytochrome C oxidase (COX) is the fourth component of the respiratory chain and is located within the internal membrane of mitochondria. COX deficiency causes an inherited mitochondrial disease with significant genetic and phenotypic heterogeneity. Four clinical subtypes have been identified, each with distinct phenotypes and genetic variants. Mitochondrial complex IV deficiency nuclear type 4 (MC4DN4) is a form of COX deficiency associated with pathogenic variants in the SCO1 gene.

CASE DESCRIPTION

We describe three patients with MC4DN4 with developmental and epileptic encephalopathy (DEE), hypopituitarism, and SCO1 pathogenic variants. These patients' phenotypes considerably differ from previously reported MC4DN4 phenotypes as they associate DEE with progressive hypopituitarism and survival beyond the first months after birth. Pituitary deficiency in these patients progressively worsened and mainly involved growth hormone secretion and thyroid function.

CONCLUSIONS

Our findings expand knowledge of phenotypic variability in MC4DN4 and suggest that SCO1 is a candidate gene for genetic hypopituitarism and DEE.

SIGNIFICANCE STATEMENT

Our paper describes three patients affected by MC4DN4 with hypopituitarism and developmental and epileptic encephalopathy (DEE), two features that have never been associated with this condition. In addition, we reviewed the clinical features of all previous cases of MC4DN4 to give the other clinicians a wide picture of the clinical phenotype of this genetic disease. We hope that the publication of our data may help others to identify this disease and consider the chance to analyze the SCO1 gene in cases of DEE associated with pituitary dysfunction. Our article contributes to expanding the spectrum of genetic hypopituitarism and proposes a model to explain an association between this condition, mitochondrial anomalies, and neurodevelopmental defects.

摘要

背景

细胞色素C氧化酶（COX）是呼吸链的第四个组成部分，位于线粒体内膜。COX缺乏会导致一种具有显著遗传和表型异质性的遗传性线粒体疾病。已确定四种临床亚型，每种亚型都有不同的表型和基因变异。线粒体复合物IV缺乏核型4（MC4DN4）是一种与SCO1基因致病性变异相关的COX缺乏形式。

病例描述

我们描述了三名患有MC4DN4且伴有发育性和癫痫性脑病（DEE）、垂体功能减退和SCO1致病性变异的患者。这些患者的表型与先前报道的MC4DN4表型有很大不同，因为他们将DEE与进行性垂体功能减退以及出生后第一个月后的存活联系起来。这些患者的垂体功能减退逐渐恶化，主要涉及生长激素分泌和甲状腺功能。

结论

我们的研究结果扩展了对MC4DN4表型变异性的认识，并表明SCO1是遗传性垂体功能减退和DEE的候选基因。

意义声明

我们的论文描述了三名受MC4DN4影响且患有垂体功能减退以及发育性和癫痫性脑病（DEE）的患者，这两种特征此前从未与该疾病相关联。此外，我们回顾了所有先前MC4DN4病例的临床特征，以便为其他临床医生提供这种遗传疾病临床表型的全面情况。我们希望我们数据的发表可能有助于其他人识别这种疾病，并考虑在与垂体功能障碍相关的DEE病例中分析SCO1基因的机会。我们的文章有助于扩大遗传性垂体功能减退的范围，并提出一个模型来解释这种疾病、线粒体异常和神经发育缺陷之间的关联。