一种独特的翻译起始机制产生用于免疫监视的隐蔽肽。

A distinct translation initiation mechanism generates cryptic peptides for immune surveillance.

作者信息

Starck Shelley R, Ow Yongkai, Jiang Vivian, Tokuyama Maria, Rivera Mark, Qi Xin, Roberts Richard W, Shastri Nilabh

机构信息

Division of Immunology and Pathogenesis, Department of Molecular and Cell Biology, University of California, Berkeley, California, United States of America.

出版信息

PLoS One. 2008;3(10):e3460. doi: 10.1371/journal.pone.0003460. Epub 2008 Oct 21.

DOI:10.1371/journal.pone.0003460

PMID:18941630

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2565129/

Abstract

MHC class I molecules present a comprehensive mixture of peptides on the cell surface for immune surveillance. The peptides represent the intracellular protein milieu produced by translation of endogenous mRNAs. Unexpectedly, the peptides are encoded not only in conventional AUG initiated translational reading frames but also in alternative cryptic reading frames. Here, we analyzed how ribosomes recognize and use cryptic initiation codons in the mRNA. We find that translation initiation complexes assemble at non-AUG codons but differ from canonical AUG initiation in response to specific inhibitors acting within the peptidyl transferase and decoding centers of the ribosome. Thus, cryptic translation at non-AUG start codons can utilize a distinct initiation mechanism which could be differentially regulated to provide peptides for immune surveillance.

摘要

MHC I类分子在细胞表面呈现出用于免疫监视的肽段的综合混合物。这些肽段代表了由内源性mRNA翻译产生的细胞内蛋白质环境。出乎意料的是，这些肽段不仅由传统的AUG起始翻译阅读框编码，还由替代的隐蔽阅读框编码。在这里，我们分析了核糖体如何识别和使用mRNA中的隐蔽起始密码子。我们发现翻译起始复合物在非AUG密码子处组装，但在响应作用于核糖体肽基转移酶和解码中心的特定抑制剂时，与典型的AUG起始不同。因此，非AUG起始密码子处的隐蔽翻译可以利用一种独特的起始机制，该机制可能受到差异调节以提供用于免疫监视的肽段。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/286d/2565129/d4a6c0b0f337/pone.0003460.g001.jpg

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一种独特的翻译起始机制产生用于免疫监视的隐蔽肽。

A distinct translation initiation mechanism generates cryptic peptides for immune surveillance.

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