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STRING v11: protein-protein association networks with increased coverage, supporting functional discovery in genome-wide experimental datasets.STRING v11:具有增强覆盖范围的蛋白质-蛋白质相互作用网络,支持在全基因组实验数据集的功能发现。
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Ribosome assembly coming into focus.核糖体组装备受关注。
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Hierarchical recruitment of ribosomal proteins and assembly factors remodels nucleolar pre-60S ribosomes.核糖体蛋白和组装因子的层次募集重塑核仁前 60S 核糖体。
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Turnover of aberrant pre-40S pre-ribosomal particles is initiated by a novel endonucleolytic decay pathway.异常的 pre-40S 前核糖体颗粒的周转率是由一种新的内切核酸酶降解途径启动的。
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Visualizing the Assembly Pathway of Nucleolar Pre-60S Ribosomes.可视化核仁前60S核糖体的组装途径。
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Reconstitution of the complete pathway of ITS2 processing at the pre-ribosome.在核前体核糖体中重建 ITS2 加工的完整途径。
Nat Commun. 2017 Nov 27;8(1):1787. doi: 10.1038/s41467-017-01786-9.
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The complete structure of the small-subunit processome.小亚基核糖体组装体的完整结构。
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Structural insights into the interaction of the nuclear exosome helicase Mtr4 with the preribosomal protein Nop53.核外切体解旋酶Mtr4与核糖体前体蛋白Nop53相互作用的结构解析
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核糖体组装因子 Nop53 控制 RNA 外切体与酵母前 60S 颗粒的结合。

The ribosome assembly factor Nop53 controls association of the RNA exosome with pre-60S particles in yeast.

机构信息

Department of Biochemistry, Institute of Chemistry, University of São Paulo, 05508-000 São Paulo, SP, Brazil.

Proteomics Unit and Laboratory of Proteomics/LADETEC, Federal University of Rio de Janeiro, 22410-001 Rio de Janeiro (RJ), Brazil.

出版信息

J Biol Chem. 2019 Dec 13;294(50):19365-19380. doi: 10.1074/jbc.RA119.010193. Epub 2019 Oct 29.

DOI:10.1074/jbc.RA119.010193
PMID:31662437
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6916480/
Abstract

Eukaryotic ribosomal biogenesis is a high-energy-demanding and complex process that requires hundreds of -acting factors to dynamically build the highly-organized 40S and 60S subunits. Each ribonucleoprotein complex comprises specific rRNAs and ribosomal proteins that are organized into functional domains. The RNA exosome complex plays a crucial role as one of the pre-60S-processing factors, because it is the RNase responsible for processing the 7S pre-rRNA to the mature 5.8S rRNA. The yeast pre-60S assembly factor Nop53 has previously been shown to associate with the nucleoplasmic pre-60S in a region containing the "foot" structure assembled around the 3' end of the 7S pre-rRNA. Nop53 interacts with 25S rRNA and with several 60S assembly factors, including the RNA exosome, specifically, with its catalytic subunit Rrp6 and with the exosome-associated RNA helicase Mtr4. Nop53 is therefore considered the adaptor responsible for recruiting the exosome complex for 7S processing. Here, using proteomics-based approaches in budding yeast to analyze the effects of Nop53 on the exosome interactome, we found that the exosome binds pre-ribosomal complexes early during the ribosome maturation pathway. We also identified interactions through which Nop53 modulates exosome activity in the context of 60S maturation and provide evidence that in addition to recruiting the exosome, Nop53 may also be important for positioning the exosome during 7S processing. On the basis of these findings, we propose that the exosome is recruited much earlier during ribosome assembly than previously thought, suggesting the existence of additional interactions that remain to be described.

摘要

真核生物核糖体生物发生是一个高能量需求和复杂的过程,需要数百种因子动态地构建高度组织化的 40S 和 60S 亚基。每个核糖核蛋白复合物包含特定的 rRNA 和核糖体蛋白,它们被组织成功能域。RNA 外切酶复合物作为前 60S 加工因子之一发挥着至关重要的作用,因为它是负责将 7S 前 rRNA 加工为成熟的 5.8S rRNA 的 RNase。酵母前 60S 组装因子 Nop53 先前已被证明与核质前 60S 结合,该区域包含围绕 7S 前 rRNA 3' 端组装的“脚”结构。Nop53 与 25S rRNA 和几个 60S 组装因子相互作用,包括 RNA 外切酶,特别是其催化亚基 Rrp6 和外切酶相关的 RNA 解旋酶 Mtr4。因此,Nop53 被认为是负责招募外切酶复合物进行 7S 加工的衔接蛋白。在这里,我们使用芽殖酵母中的基于蛋白质组学的方法来分析 Nop53 对 exosome 相互作用组的影响,我们发现外切酶在核糖体成熟途径的早期结合前核糖体复合物。我们还通过鉴定 Nop53 在 60S 成熟过程中调节外切酶活性的相互作用,提供了证据表明,除了招募外切酶外,Nop53 在外切酶 7S 加工过程中可能也对定位外切酶很重要。基于这些发现,我们提出外切酶在核糖体组装过程中比以前认为的更早被招募,这表明存在其他有待描述的相互作用。