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核糖体上的肽释放:机制及其对翻译控制的影响

Peptide release on the ribosome: mechanism and implications for translational control.

作者信息

Youngman Elaine M, McDonald Megan E, Green Rachel

机构信息

Howard Hughes Medical Institute, Department of Molecular Biology and Genetics, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205, USA.

出版信息

Annu Rev Microbiol. 2008;62:353-73. doi: 10.1146/annurev.micro.61.080706.093323.

Abstract

Peptide release, the reaction that hydrolyzes a completed protein from the peptidyl-tRNA upon completion of translation, is catalyzed in the active site of the large subunit of the ribosome and requires a class I release factor protein. The ribosome and release factor protein cooperate to accomplish two tasks: recognition of the stop codon and catalysis of peptidyl-tRNA hydrolysis. Although many fundamental questions remain, substantial progress has been made in the past several years. This review summarizes those advances and presents current models for the mechanisms of stop codon specificity and catalysis of peptide release. Finally, we discuss how these views fit into a larger emerging theme in the translation field: the importance of induced fit and conformational changes for progression through the translation cycle.

摘要

肽释放是指在翻译完成后从肽基 - tRNA水解完整蛋白质的反应,该反应在核糖体大亚基的活性位点被催化,并且需要I类释放因子蛋白。核糖体和释放因子蛋白协同完成两项任务:识别终止密码子和催化肽基 - tRNA水解。尽管仍有许多基本问题有待解决,但在过去几年中已经取得了实质性进展。本综述总结了这些进展,并提出了目前关于终止密码子特异性机制和肽释放催化的模型。最后,我们讨论这些观点如何融入翻译领域一个更大的新出现的主题:诱导契合和构象变化对翻译循环进程的重要性。

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