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协同的结构重排使 RNA 通道进入细胞质 Ski238-Ski7-exosome 组装。

Concerted structural rearrangements enable RNA channeling into the cytoplasmic Ski238-Ski7-exosome assembly.

机构信息

Department of Structural Cell Biology, Max Planck Institute of Biochemistry, Am Klopferspitz 18, Martinsried, 82152 Munich, Germany.

EMBL Grenoble, 71 Avenue des Martyrs, 38072 Grenoble, France.

出版信息

Mol Cell. 2023 Nov 16;83(22):4093-4105.e7. doi: 10.1016/j.molcel.2023.09.037. Epub 2023 Oct 24.

Abstract

The Ski2-Ski3-Ski8 (Ski238) helicase complex directs cytoplasmic mRNAs toward the nucleolytic exosome complex for degradation. In yeast, the interaction between Ski238 and exosome requires the adaptor protein Ski7. We determined different cryo-EM structures of the Ski238 complex depicting the transition from a rigid autoinhibited closed conformation to a flexible active open conformation in which the Ski2 helicase module has detached from the rest of Ski238. The open conformation favors the interaction of the Ski3 subunit with exosome-bound Ski7, leading to the recruitment of the exosome. In the Ski238-Ski7-exosome holocomplex, the Ski2 helicase module binds the exosome cap, enabling the RNA to traverse from the helicase through the internal exosome channel to the Rrp44 exoribonuclease. Our study pinpoints how conformational changes within the Ski238 complex regulate exosome recruitment for RNA degradation. We also reveal the remarkable conservation of helicase-exosome RNA channeling mechanisms throughout eukaryotic nuclear and cytoplasmic exosome complexes.

摘要

Ski2-Ski3-Ski8(Ski238)解旋酶复合物将细胞质 mRNA 导向核酶体复合物进行降解。在酵母中,Ski238 与核酶体的相互作用需要衔接蛋白 Ski7。我们确定了 Ski238 复合物的不同 cryo-EM 结构,这些结构描绘了从刚性的自动抑制的封闭构象到灵活的活性开放构象的转变,在这种开放构象中,Ski2 解旋酶模块已从 Ski238 的其余部分脱离。开放构象有利于 Ski3 亚基与结合 Ski7 的核酶体的相互作用,导致核酶体的募集。在 Ski238-Ski7-核酶体全复合物中,Ski2 解旋酶模块结合核酶体盖帽,使 RNA 能够从解旋酶通过内部核酶体通道到达 Rrp44 外切核酸酶。我们的研究指出了 Ski238 复合物内的构象变化如何调节核酶体的募集以进行 RNA 降解。我们还揭示了整个真核核和细胞质核酶体复合物中解旋酶-核酶体 RNA 通道机制的显著保守性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e6ba/10659929/8f3693ea1151/fx1.jpg

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