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酵母 Puf3p 家族蛋白 Puf3p 对线粒体翻译、呼吸和代谢周期调节基因 SLF1 的抑制作用。

Repression of mitochondrial translation, respiration and a metabolic cycle-regulated gene, SLF1, by the yeast Pumilio-family protein Puf3p.

机构信息

Department of Pathology, Yale University School of Medicine, New Haven, Connecticut, United States of America.

出版信息

PLoS One. 2011;6(5):e20441. doi: 10.1371/journal.pone.0020441. Epub 2011 May 31.

Abstract

Synthesis and assembly of the mitochondrial oxidative phosphorylation (OXPHOS) system requires genes located both in the nuclear and mitochondrial genomes, but how gene expression is coordinated between these two compartments is not fully understood. One level of control is through regulated expression mitochondrial ribosomal proteins and other factors required for mitochondrial translation and OXPHOS assembly, which are all products of nuclear genes that are subsequently imported into mitochondria. Interestingly, this cadre of genes in budding yeast has in common a 3'-UTR element that is bound by the Pumilio family protein, Puf3p, and is coordinately regulated under many conditions, including during the yeast metabolic cycle. Multiple functions have been assigned to Puf3p, including promoting mRNA degradation, localizing nucleus-encoded mitochondrial transcripts to the outer mitochondrial membrane, and facilitating mitochondria-cytoskeletal interactions and motility. Here we show that Puf3p has a general repressive effect on mitochondrial OXPHOS abundance, translation, and respiration that does not involve changes in overall mitochondrial biogenesis and largely independent of TORC1-mitochondrial signaling. We also identified the cytoplasmic translation factor Slf1p as yeast metabolic cycle-regulated gene that is repressed by Puf3p at the post-transcriptional level and promotes respiration and extension of yeast chronological life span when over-expressed. Altogether, these results should facilitate future studies on which of the many functions of Puf3p is most relevant for regulating mitochondrial gene expression and the role of nuclear-mitochondrial communication in aging and longevity.

摘要

线粒体氧化磷酸化(OXPHOS)系统的合成和组装需要位于核基因组和线粒体基因组中的基因,但基因表达如何在这两个隔室之间协调尚不完全清楚。一种控制水平是通过调节核基因编码的线粒体核糖体蛋白和其他用于线粒体翻译和 OXPHOS 组装的因子的表达来实现的,这些基因随后被导入线粒体。有趣的是,在 budding yeast 中,这一组基因都有一个 3'-UTR 元件,该元件被 Pumilio 家族蛋白 Puf3p 结合,并在许多条件下(包括在酵母代谢周期中)被协调调节。Puf3p 具有多种功能,包括促进 mRNA 降解、将核编码的线粒体转录物定位于外线粒体膜、促进线粒体-细胞骨架相互作用和运动。在这里,我们表明 Puf3p 对线粒体 OXPHOS 丰度、翻译和呼吸具有普遍的抑制作用,不涉及整体线粒体生物发生的变化,并且在很大程度上独立于 TORC1-线粒体信号。我们还鉴定了细胞质翻译因子 Slf1p 作为酵母代谢周期调节基因,它在转录后水平被 Puf3p 抑制,并在过表达时促进呼吸和延长酵母的时序寿命。总之,这些结果应该有助于未来研究 Puf3p 的许多功能中哪些与调节线粒体基因表达最相关,以及核-线粒体通讯在衰老和长寿中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6790/3105058/b5241865191d/pone.0020441.g001.jpg

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