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The mRNA export machinery requires the novel Sac3p–Thp1p complex to dock at the nucleoplasmic entrance of the nuclear pores

机译：mRNA输出机制需要新型Sac3p–Thp1p复合物停靠在核孔的核质入口

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摘要

Yra1p and Sub2p are components of the TREX complex, which couples transcription elongation with nuclear export of mRNAs. Here, we report a genetic interaction between Yra1p and a conserved protein Sac3p, which previously was found to interact with Sub2p. In vivo, Sac3p forms a stable complex with Thp1p, which was reported to function in transcription elongation. In addition, Sac3p binds to the mRNA exporter Mex67p–Mtr2p and requires the nucleoporin Nup1p to dock at the nuclear side of the nuclear pore complex (NPC). Significantly, mutations in Sac3p or Thp1p lead to strong mRNA export defects. Taken together, our data suggest that the novel Sac3p–Thp1p complex functions by docking the mRNP to specific nucleoporins at the nuclear entrance of the NPC.

机译：Yra1p和Sub2p是TREX复合体的组成部分，该复合体将转录延长与mRNA的核输出耦合。在这里，我们报告Yra1p和保守的蛋白Sac3p之间的遗传相互作用，以前发现该蛋白与Sub2p相互作用。在体内，Sac3p与Thp1p形成稳定的复合物，据报道在转录延伸中起作用。此外，Sac3p与mRNA出口子Mex67p–Mtr2p结合，需要核孔蛋白Nup1p停靠在核孔复合体（NPC）的核侧。显然，Sac3p或Thp1p中的突变会导致强烈的mRNA输出缺陷。两者合计，我们的数据表明，新型Sac3p–Thp1p复合体通过将mRNP停靠在NPC核入口处的特定核孔蛋白上而发挥功能。

著录项

期刊名称 The EMBO Journal
作者
Tamás Fischer; Katja Sträßer; Attila Rácz; Susana Rodriguez-Navarro; Marisa Oppizzi; Petra Ihrig; Johannes Lechner; Ed Hurt;
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作者单位

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年(卷),期 2002(21),21
年度 2002
页码 5843–5852
总页数 10
原文格式 PDF
正文语种
中图分类分子生物学;细胞生物学;
关键词
Mex67p/mRNA exportuclear pore complexucleoporin/Sac3p;

机译：Mex67p / mRNA出口/核孔复合物/核孔蛋白/ Sac3p;

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专利

1. Nuclear mRNA Export Requires Specific FG Nucleoporins for Translocation Through the Nuclear Pore Complex [J] . Howard M. Fried Chemtracts . 2007,第4期

机译：核mRNA出口需要特定的FG Nucleoporins通过核孔复合体易位。
2. Nuclear mRNA export requires specific FG nucleoporins for translocation through the nuclear pore complex [J] . Laura J. Terry, Susan R. Wente Journal of cell biology . 2007,第7期

机译：核mRNA输出需要特定的FG核孔蛋白才能通过核孔复合体转运
3. Nuclear mRNA Export Requires Complex Formation between Mex67p and Mtr2p at the Nuclear Pores [J] . Helena Santos-Rosa, Horacio Moreno, George Simos, Molecular and Cellular Biology . 1998,第11期

机译：核mRNA出口需要核孔中Mex67p和Mtr2p之间的复杂形成。
4. PORE-SCALE NUMERICAL MODELING OF NUCLEAR MAGNETIC RESONANCE RESPONSE IN ROCKS WITH COMPLEX PORE STRUCTURE USING FINITE VOLUME METHOD [C] . Saurabh Tandon, Zoya Heidari, Grigorios Matenoglou SPWLA annual logging symposium;Society of Petrophysicists and Well Log Analysts, inc . 2017

机译：复杂体积结构岩石中核磁共振响应的大尺度数值模拟的有限体积法
5. Cex1p is a novel component of the Saccharomyces cerevisiae nuclear tRNA export machinery that facilitates dissociation of the tRNA-export receptor complex at the cytoplasmic face of the nuclear pore complex. [D] . McGuire, Andrew T. 2011

机译：Cex1p是啤酒酵母核tRNA出口机制的新型组件，可促进tRNA出口受体复合物在核孔复合体的胞质面上解离。
6. Influenza virus targets the mRNA export machinery and the nuclear pore complex [O] . Neal Satterly, Pei-Ling Tsai, Jan van Deursen, 2007

机译：流感病毒靶向mRNA输出机器和核孔复合体
7. The mRNA export machinery requires the novel Sac3p-Thp1p complex to dock at the nucleoplasmic entrance of the nuclear pores [O] . T. Fischer 2002

机译：MRNA出口机制需要新型SAC3P-THP1P复合物在核毛孔的核状入口处码头

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