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阐明 Utp20、Imp4 和 Bms1 招募到新生前核糖体上所需的组装事件。

Elucidation of the assembly events required for the recruitment of Utp20, Imp4 and Bms1 onto nascent pre-ribosomes.

机构信息

Centro de Investigación del Cáncer and Instituto de Biología Molecular y Celular del Cáncer, CSIC-University of Salamanca, Campus Unamuno s/n, E37007 Salamanca, Spain.

出版信息

Nucleic Acids Res. 2011 Oct;39(18):8105-21. doi: 10.1093/nar/gkr508. Epub 2011 Jun 30.

Abstract

The 90S pre-ribosome, also known as the small subunit (SSU) processome, is a large multisubunit particle required for the production of the 18S rRNA from a pre-rRNA precursor. Recently, it has been shown that the formation of this particle entails the initial association of the tUTP subunit with the nascent pre-RNA and, subsequently, the binding of Rrp5/UTP-C and U3 snoRNP/UTP-B subunits in two independent assembly branches. However, the mode of assembly of other 90S pre-ribosome components remains obscure as yet. In this study, we have investigated the assembly of three proteins (Utp20, Imp4 and Bms1) previously regarded as potential nucleating factors of the 90S particle. Here, we demonstrate that the loading of those three proteins onto the pre-rRNA takes place independently of Rrp5/UTP-C and, instead, occurs downstream of the tUTP and U3/UTP-B subcomplexes. We also demonstrate that Bms1 and Utp20 are required for the recruitment of a subset of proteins to nascent pre-ribosomes. Finally, we show that proteins associated through secondary steps condition the stability of the two assembly branches in partially assembled pre-ribosomes. These results provide new information about the functional relationships among 90S particle components and the events that are required for their stepwise incorporation onto the primary pre-rRNA.

摘要

90S 前核糖体,也称为小亚基(SSU)加工体,是一个大型多亚基颗粒,对于从前 rRNA 前体产生 18S rRNA 是必需的。最近,已经表明该颗粒的形成需要 tUTP 亚基与新生前 RNA 的初始结合,随后,Rrp5/UTP-C 和 U3 snoRNP/UTP-B 亚基在两个独立的组装分支中结合。然而,其他 90S 前核糖体成分的组装方式仍然不清楚。在这项研究中,我们研究了三个以前被认为是 90S 颗粒形成核因子的蛋白质(Utp20、Imp4 和 Bms1)的组装。在这里,我们证明这三种蛋白质加载到 pre-rRNA 上的过程独立于 Rrp5/UTP-C,而是发生在 tUTP 和 U3/UTP-B 亚基复合物之后。我们还证明 Bms1 和 Utp20 对于一组蛋白质向新生前核糖体的募集是必需的。最后,我们表明通过二级步骤相关的蛋白质条件部分组装的前核糖体中两个组装分支的稳定性。这些结果提供了关于 90S 颗粒成分之间的功能关系以及它们逐步整合到初级 pre-rRNA 所需的事件的新信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0250/3185420/2bca865d9b50/gkr508f1.jpg

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