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Structure of the nuclear exosome captured on a maturing preribosome.核小体在成熟前核糖体上的捕获结构。
Science. 2018 Apr 13;360(6385):219-222. doi: 10.1126/science.aar5428. Epub 2018 Mar 8.
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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。
Cell. 2017 Dec 14;171(7):1599-1610.e14. doi: 10.1016/j.cell.2017.11.039.
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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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3.2-Å-resolution structure of the 90S preribosome before A1 pre-rRNA cleavage.90S 前核糖体在 A1 前 rRNA 切割前的 3.2-Å 分辨率结构。
Nat Struct Mol Biol. 2017 Nov;24(11):954-964. doi: 10.1038/nsmb.3476. Epub 2017 Oct 2.
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Comparison of preribosomal RNA processing pathways in yeast, plant and human cells - focus on coordinated action of endo- and exoribonucleases.酵母、植物和人类细胞中前核糖体RNA加工途径的比较——聚焦于内切核糖核酸酶和外切核糖核酸酶的协同作用。
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Targeted CRISPR disruption reveals a role for RNase MRP RNA in human preribosomal RNA processing.靶向CRISPR干扰揭示了核糖核酸酶MRP RNA在人类前体核糖体RNA加工中的作用。
Genes Dev. 2017 Jan 1;31(1):59-71. doi: 10.1101/gad.286963.116. Epub 2017 Jan 23.
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The interaction of a Trypanosoma brucei KH-domain protein with a ribonuclease is implicated in ribosome processing.布氏锥虫KH结构域蛋白与核糖核酸酶的相互作用与核糖体加工有关。
Mol Biochem Parasitol. 2017 Jan;211:94-103. doi: 10.1016/j.molbiopara.2016.12.003. Epub 2016 Dec 11.
8
Nuclear RNA Exosome at 3.1 Å Reveals Substrate Specificities, RNA Paths, and Allosteric Inhibition of Rrp44/Dis3.3.1埃分辨率下的核RNA外切体复合物揭示了Rrp44/Dis3的底物特异性、RNA路径和变构抑制作用。
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Architecture of the 90S Pre-ribosome: A Structural View on the Birth of the Eukaryotic Ribosome.90S 前核糖体的结构:真核核糖体诞生的结构视角。
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Gene expression in Kinetoplastids.动质体中的基因表达。
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布氏锥虫 RRP44 参与大亚基核糖体 RNA 成熟的早期阶段。

Trypanosoma brucei RRP44 is involved in an early stage of large ribosomal subunit RNA maturation.

机构信息

a Carlos Chagas Institute , Oswaldo Cruz Foundation, FIOCRUZ-PR , Curitiba , Brazil.

b Biochemsitry Postgraduate Program , Federal University of Parana , Curitiba , Brazil.

出版信息

RNA Biol. 2019 Jan;16(1):133-143. doi: 10.1080/15476286.2018.1564463. Epub 2019 Jan 7.

DOI:10.1080/15476286.2018.1564463
PMID:30593255
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6380303/
Abstract

Ribosomal RNA precursors undergo a series of structural and chemical modifications to generate matured RNA molecules that will comprise ribosomes. This maturation process involves a large set of accessory proteins as well as ribonucleases, responsible for removal of the external and internal transcribed spacers from the pre-rRNA. Early-diverging eukaryotes belonging to the Kinetoplastida class display several unique characteristics, in particular in terms of RNA synthesis and maturation. These peculiarities include the rRNA biogenesis and the extensive fragmentation of the large ribosomal subunit (LSU) rRNA. The role of specific endo- and exonucleases in the maturation of the unusual rRNA precursor of trypanosomatids remains largely unknown. One of the nucleases involved in rRNA processing is Rrp44, an exosome associated ribonuclease in yeast, which is involved in several metabolic RNA pathways. Here, we investigated the function of Trypanosoma brucei RRP44 orthologue (TbRRP44) in rRNA processing. Our results revealed that TbRRP44 depletion causes unusual polysome profile and accumulation of the complete LSU rRNA precursor, in addition to 5.8S maturation impairment. We also determined the crystal structure of TbRRP44 endonucleolytic domain. Structural comparison with Saccharomyces cerevisiae Rrp44 revealed differences in the catalytic site and substitutions of surface residues, which could provide molecular bases for the lack of interaction of RRP44 with the exosome complex in T. brucei.

摘要

核糖体 RNA 前体经历一系列结构和化学修饰,生成成熟的 RNA 分子,这些成熟的 RNA 分子将构成核糖体。这个成熟过程涉及一大组辅助蛋白和核糖核酸酶,负责从 pre-rRNA 中去除外部和内部转录间隔区。属于动基体门的早期真核生物表现出一些独特的特征,特别是在 RNA 合成和成熟方面。这些特点包括 rRNA 的生物发生和大亚基(LSU)rRNA 的广泛断裂。特定内切核酸酶和外切核酸酶在锥虫 rRNA 前体的成熟中的作用在很大程度上仍然未知。参与 rRNA 加工的核酸酶之一是 Rrp44,它是酵母中与 exosome 相关的核糖核酸酶,参与多种代谢 RNA 途径。在这里,我们研究了参与 rRNA 加工的 Trypanosoma brucei RRP44 同源物(TbRRP44)的功能。我们的结果表明,TbRRP44 耗尽会导致异常的多核糖体图谱和完整 LSU rRNA 前体的积累,除了 5.8S 成熟受损。我们还确定了 TbRRP44 内切核酸酶结构域的晶体结构。与酿酒酵母 Rrp44 的结构比较显示,催化位点和表面残基的取代存在差异,这可能为 T. brucei 中 RRP44 与 exosome 复合物缺乏相互作用提供分子基础。