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Argonautes 与 alpha-sarcin 样核糖核酸酶之间的相似性:对 microRNA 作用的启示。

Similarities between Argonautes and the alpha-sarcin-like ribotoxins: Implications for microRNA action.

机构信息

Department of Cell Research and Immunology, Tel Aviv University, Ramat Aviv 69978, Israel.

出版信息

Protein Sci. 2010 Jun;19(6):1272-8. doi: 10.1002/pro.391.

Abstract

We report structural, functional, and biochemical similarities between Argonautes, the effector proteins of RNA-induced silencing complexes (RISCs), and alpha-sarcin-like ribotoxins. At the structural level, regions of similarity in the amino acid sequence are located in protein loops both in the ribotoxins and in the Argonautes. In ribotoxins, these protein loops confer specificity for a highly conserved segment of ribosomal RNA, the Sarcin-Ricin-Loop (SRL) that undergoes cleavage by the ribotoxin ribonuclease. This leads to suppression of translation. In addition to the structural similarity with ribotoxins, the Argonaute proteins (Ago) show both functional and biochemical parallels. Like the ribotoxins, the Agos exhibit ribonuclease activity and like the ribotoxins, translational suppression mediated by miRISC-resident Ago is accompanied by intact polysomes. Furthermore, in both translationally suppressed systems, the puromycin reaction, reflecting correct translocation and peptidyl-transferase activities, is unharmed. These findings support a mechanism for Ago-miRISCs whereby regulated cleavage of ribosomal RNA leads to translational suppression.

摘要

我们报告 Argonautes(RNA 诱导沉默复合物的效应蛋白)与 α-亚精胺酶样核糖核酸酶之间在结构、功能和生化方面的相似性。在结构水平上,核糖核酸酶和 Argonautes 中氨基酸序列相似的区域位于蛋白质环中。在核糖核酸酶中,这些蛋白质环赋予其对核糖体 RNA 高度保守片段(Sarcin-Ricin-Loop,SRL)的特异性,该片段会被核糖核酸酶切割,从而抑制翻译。除了与核糖核酸酶的结构相似性外,Argonaute 蛋白(Ago)还表现出功能和生化方面的相似性。与核糖核酸酶一样,Agos 表现出核糖核酸酶活性,并且像核糖核酸酶一样,miRISC 驻留的 Ago 介导的翻译抑制伴随着完整的多核糖体。此外,在这两种翻译抑制系统中,对氨苯砜反应,反映正确的易位和肽基转移酶活性,没有受到损害。这些发现支持 Ago-miRISCs 的一种机制,即通过调节核糖体 RNA 的切割来导致翻译抑制。

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Argonaute proteins: key players in RNA silencing.Argonaute蛋白:RNA沉默的关键参与者。
Nat Rev Mol Cell Biol. 2008 Jan;9(1):22-32. doi: 10.1038/nrm2321.

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