Proteolytic regulation of mitochondrial magnesium channel MRS2 by m-AAA protease and prohibitin complex.

IF 3.3 3区 生物学 Q2 GENETICS & HEREDITY
Genetics Pub Date : 2024-12-05 DOI:10.1093/genetics/iyae203
Alaumy Joshi, Rachel A Stanfield, Andrew T Spletter, Vishal M Gohil
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引用次数: 0

Abstract

Mitochondrial membrane phospholipid cardiolipin is essential for the stability of several inner mitochondrial membrane protein complexes. We recently showed that the abundance of mitochondrial magnesium channel MRS2 is reduced in models of Barth syndrome, an X-linked genetic disorder caused by a remodeling defect in cardiolipin. However, the mechanism underlying the reduced abundance of MRS2 in cardiolipin-depleted mitochondria remained unknown. In this study, we utilized yeast mutants of mitochondrial proteases to identify an evolutionarily conserved m-AAA protease, Yta10/Yta12, responsible for degrading Mrs2. The activity of m-AAA protease is regulated by the inner mitochondrial membrane scaffolding complex prohibitin, and consistent with this role, we find that Mrs2 turnover is increased in yeast prohibitin mutants. Importantly, we find that deleting Yta10 in cardiolipin-deficient yeast cells restores the steady-state levels of Mrs2 to the wild-type cells, and the knockdown of AFG3L2, a mammalian homolog of Yta12, increases the abundance of MRS2 in a murine muscle cell line. Thus, our work has identified the m-AAA protease/prohibitin complex as an evolutionarily conserved regulator of Mrs2 that can be targeted to restore Mrs2 abundance in cardiolipin-depleted cells.

m-AAA蛋白酶和禁止素复合体对线粒体镁通道MRS2的蛋白水解调控。
线粒体膜磷脂心磷脂对多个线粒体内膜蛋白复合物的稳定性至关重要。我们最近发现,在巴特综合征模型中,线粒体镁通道MRS2的丰度会降低,巴特综合征是一种由心磷脂重塑缺陷引起的X连锁遗传疾病。然而,MRS2 在缺失心磷脂的线粒体中丰度降低的机制仍然未知。在这项研究中,我们利用线粒体蛋白酶的酵母突变体鉴定了负责降解 Mrs2 的进化保守的 m-AAA 蛋白酶 Yta10/Yta12。m-AAA 蛋白酶的活性受线粒体内膜支架复合物 prohibitin 的调控,与这一作用相一致,我们发现酵母 prohibitin 突变体中 Mrs2 的周转率增加。重要的是,我们发现在心磷脂缺乏的酵母细胞中删除 Yta10 可使 Mrs2 的稳态水平恢复到野生型细胞的水平,而在小鼠肌肉细胞系中敲除 Yta12 的哺乳动物同源物 AFG3L2 可增加 MRS2 的丰度。因此,我们的研究发现,m-AAA 蛋白酶/抑制素复合物是 Mrs2 在进化过程中保守的调控因子,可以作为靶点恢复心磷脂耗竭细胞中 Mrs2 的丰度。
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来源期刊
Genetics
Genetics GENETICS & HEREDITY-
CiteScore
6.90
自引率
6.10%
发文量
177
审稿时长
1.5 months
期刊介绍: GENETICS is published by the Genetics Society of America, a scholarly society that seeks to deepen our understanding of the living world by advancing our understanding of genetics. Since 1916, GENETICS has published high-quality, original research presenting novel findings bearing on genetics and genomics. The journal publishes empirical studies of organisms ranging from microbes to humans, as well as theoretical work. While it has an illustrious history, GENETICS has changed along with the communities it serves: it is not your mentor''s journal. The editors make decisions quickly – in around 30 days – without sacrificing the excellence and scholarship for which the journal has long been known. GENETICS is a peer reviewed, peer-edited journal, with an international reach and increasing visibility and impact. All editorial decisions are made through collaboration of at least two editors who are practicing scientists. GENETICS is constantly innovating: expanded types of content include Reviews, Commentary (current issues of interest to geneticists), Perspectives (historical), Primers (to introduce primary literature into the classroom), Toolbox Reviews, plus YeastBook, FlyBook, and WormBook (coming spring 2016). For particularly time-sensitive results, we publish Communications. As part of our mission to serve our communities, we''ve published thematic collections, including Genomic Selection, Multiparental Populations, Mouse Collaborative Cross, and the Genetics of Sex.
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