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一个位于 LYRM7/MZM1L 的纯合突变与早发性脑病、乳酸性酸中毒和线粒体复合物 III 活性严重降低有关。

A homozygous mutation in LYRM7/MZM1L associated with early onset encephalopathy, lactic acidosis, and severe reduction of mitochondrial complex III activity.

机构信息

Unit of Molecular Neurogenetics, Fondazione IRCCS (Istituto di Ricovero e Cura a Carattere Scientifico) Istituto Neurologico "Carlo Besta", Milan, Italy.

出版信息

Hum Mutat. 2013 Dec;34(12):1619-22. doi: 10.1002/humu.22441. Epub 2013 Sep 23.

Abstract

Mutations in nuclear genes associated with defective complex III (cIII) of the mitochondrial respiratory chain are rare, having been found in only two cIII assembly factors and, as private changes in single families, three cIII structural subunits. Recently, human LYRM7/MZM1L, the ortholog of yeast MZM1, has been identified as a new assembly factor for cIII. In a baby patient with early onset, severe encephalopathy, lactic acidosis and profound, isolated cIII deficiency in skeletal muscle, we identified a disease-segregating homozygous mutation (c.73G>A) in LYRM7/MZM1L, predicting a drastic change in a highly conserved amino-acid residue (p.Asp25Asn). In a mzm1Δ yeast strain, the expression of a mzm1(D25N) mutant allele caused temperature-sensitive respiratory growth defect, decreased oxygen consumption, impaired maturation/stabilization of the Rieske Fe-S protein, and reduced complex III activity and amount. LYRM7/MZM1L is a novel disease gene, causing cIII-defective, early onset, severe mitochondrial encephalopathy.

摘要

与线粒体呼吸链缺陷复合 III(cIII)相关的核基因突变很少见,仅在两种 cIII 组装因子中发现,并且作为单个家族的私有变化,在三种 cIII 结构亚基中发现。最近,人类 LYRM7/MZM1L,酵母 MZM1 的同源物,被鉴定为 cIII 的新组装因子。在一名患有早发性、严重脑病、乳酸性酸中毒和骨骼肌中严重、孤立的 cIII 缺乏的婴儿患者中,我们在 LYRM7/MZM1L 中发现了一个与疾病分离的纯合突变(c.73G>A),预测高度保守的氨基酸残基(p.Asp25Asn)发生剧烈变化。在 mzm1Δ 酵母菌株中,mzm1(D25N)突变等位基因的表达导致温度敏感的呼吸生长缺陷、耗氧量降低、抑制 Rieske Fe-S 蛋白的成熟/稳定,并降低复合物 III 的活性和数量。LYRM7/MZM1L 是一种新的疾病基因,导致 cIII 缺陷、早发性、严重的线粒体脑病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1e67/4028993/054ccb22bc34/humu0034-1619-f1.jpg

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