Laboratorio de enfermedades mitocondriales, Centro de Investigación, Hospital Universitario 12 de Octubre, Madrid, Spain.
Mitochondrion. 2010 Jun;10(4):362-8. doi: 10.1016/j.mito.2010.03.003. Epub 2010 Mar 19.
The aim of this study was to identify the causative genetic lesion in two apparently unrelated newborns having lethal lactic acidosis, multi-organ failure and congenital malformations including interrupted aortic arch, who exhibited mild methylmalonic aciduria, combined mitochondrial respiratory chain deficiency, and marked muscle mitochondrial DNA depletion. A novel mutation in the SUCLG1 gene was identified. Phenotype severity in Succinate-CoA ligase dysfunction appears to be more correlated to the muscle mtDNA content than to the tissue distribution of the heterodimer subunits. Prominent impairment of mitochondrial respiratory chain may result in deep ravages in developmental tissues leading to multiple organ failure and malformations.
本研究旨在鉴定两名无明显关联的新生儿致死性乳酸酸中毒、多器官衰竭和先天性畸形(包括主动脉弓中断)的致病遗传缺陷,他们表现出轻度甲基丙二酸尿症、线粒体呼吸链复合缺陷和显著的肌肉线粒体 DNA 耗竭。鉴定到 SUCLG1 基因的一种新突变。琥珀酰辅酶 A 连接酶功能障碍的表型严重程度似乎与肌肉 mtDNA 含量更相关,而与异二聚体亚基的组织分布无关。线粒体呼吸链的显著损伤可能导致发育组织的严重破坏,导致多器官衰竭和畸形。
