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带辅因子和修饰的线粒体核糖体结构揭示了配体结合的机制以及与 L1 茎部的相互作用。

Mitoribosome structure with cofactors and modifications reveals mechanism of ligand binding and interactions with L1 stalk.

机构信息

Science for Life Laboratory, Department of Biochemistry and Biophysics, Stockholm University, 17165, Solna, Sweden.

Department of Biological Sciences, Graduate School of Science, University of Tokyo, 113-0033, Tokyo, Japan.

出版信息

Nat Commun. 2024 May 20;15(1):4272. doi: 10.1038/s41467-024-48163-x.

Abstract

The mitoribosome translates mitochondrial mRNAs and regulates energy conversion that is a signature of aerobic life forms. We present a 2.2 Å resolution structure of human mitoribosome together with validated mitoribosomal RNA (rRNA) modifications, including aminoacylated CP-tRNA. The structure shows how mitoribosomal proteins stabilise binding of mRNA and tRNA helping to align it in the decoding center, whereas the GDP-bound mS29 stabilizes intersubunit communication. Comparison between different states, with respect to tRNA position, allowed us to characterize a non-canonical L1 stalk, and molecular dynamics simulations revealed how it facilitates tRNA transitions in a way that does not require interactions with rRNA. We also report functionally important polyamines that are depleted when cells are subjected to an antibiotic treatment. The structural, biochemical, and computational data illuminate the principal functional components of the translation mechanism in mitochondria and provide a description of the structure and function of the human mitoribosome.

摘要

线粒体核糖体翻译线粒体 mRNA,并调节能量转换,这是需氧生命形式的特征。我们呈现了一个 2.2Å 分辨率的人线粒体核糖体结构,以及经过验证的线粒体核糖体 RNA(rRNA)修饰,包括氨酰化 CP-tRNA。该结构显示了线粒体核糖体蛋白如何稳定 mRNA 和 tRNA 的结合,帮助其在解码中心对齐,而 GDP 结合的 mS29 稳定了亚基间的通讯。通过比较不同状态下 tRNA 的位置,我们能够对非典型的 L1 茎进行特征描述,分子动力学模拟揭示了它如何以不依赖于 rRNA 相互作用的方式促进 tRNA 的转变。我们还报告了具有功能重要性的多胺,当细胞受到抗生素处理时,这些多胺会被耗尽。结构、生化和计算数据阐明了线粒体翻译机制的主要功能组件,并提供了人线粒体核糖体的结构和功能描述。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4b86/11106087/89c6c1868d7a/41467_2024_48163_Fig1_HTML.jpg

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