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可变起始密码子的选择在进化、体内平衡和疾病过程中塑造线粒体功能。

Alternative start codon selection shapes mitochondrial function during evolution, homeostasis, and disease.

作者信息

Ly Jimmy, Tao Yi Fei, Di Bernardo Matteo, Khalizeva Ekaterina, Giuliano Christopher J, Lourido Sebastian, Fleming Mark D, Cheeseman Iain M

机构信息

Whitehead Institute for Biomedical Research, Cambridge, United States.

Department of Biology, Massachusetts Institute of Technology, Cambridge, United States.

出版信息

bioRxiv. 2025 Mar 27:2025.03.27.645657. doi: 10.1101/2025.03.27.645657.

Abstract

Mitochondrial endosymbiosis was a pivotal event in eukaryotic evolution, requiring core proteins to adapt to function both within the mitochondria and in the host cell. Here, we systematically profile the localization of protein isoforms generated by alternate start codon selection during translation. We identify hundreds of pairs of differentially-localized protein isoforms, many of which affect mitochondrial targeting and are essential for mitochondrial function. The emergence of dual-localized mitochondrial protein isoforms coincides with mitochondrial acquisition during early eukaryotic evolution. We further reveal that eukaryotes use diverse mechanisms-such as leaky ribosome scanning, alternative transcription, and paralog duplication-to maintain the production of dual-localized isoforms. Finally, we identify multiple isoforms that are specifically dysregulated by rare disease patient mutations and demonstrate how these mutations can help explain unique clinical presentations. Together, our findings illuminate the evolutionary and pathological relevance of alternative translation initiation, offering new insights into the molecular underpinnings of mitochondrial biology.

摘要

线粒体内共生是真核生物进化中的一个关键事件,需要核心蛋白适应在线粒体和宿主细胞内发挥功能。在这里,我们系统地分析了翻译过程中由可变起始密码子选择产生的蛋白质异构体的定位。我们鉴定出数百对差异定位的蛋白质异构体,其中许多影响线粒体靶向,并且对线粒体功能至关重要。双定位线粒体蛋白质异构体的出现与早期真核生物进化过程中的线粒体获得相吻合。我们进一步揭示,真核生物使用多种机制——如核糖体扫描泄漏、可变转录和旁系同源基因复制——来维持双定位异构体的产生。最后,我们鉴定出多种因罕见病患者突变而特异性失调的异构体,并展示了这些突变如何有助于解释独特的临床表现。总之,我们的发现阐明了可变翻译起始的进化和病理相关性,为线粒体生物学的分子基础提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ce9c/11974929/3ded3373d017/nihpp-2025.03.27.645657v1-f0001.jpg

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