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dsRBP 蛋白 Staufen2 调控神经元 Argonaute 蛋白的 RNP 组装。

The dsRBP Staufen2 governs RNP assembly of neuronal Argonaute proteins.

机构信息

Biomedical Center (BMC), Department for Cell Biology, Medical Faculty, Ludwig-Maximilians-University of Munich, 82152 Planegg-Martinsried, Germany.

Core Facilities, Medical University of Vienna, 1090 Vienna, Austria.

出版信息

Nucleic Acids Res. 2022 Jul 8;50(12):7034-7047. doi: 10.1093/nar/gkac487.

Abstract

Mature microRNAs are bound by a member of the Argonaute (Ago1-4) protein family, forming the core of the RNA-induced silencing complex (RISC). Association of RISC with target mRNAs results in ribonucleoprotein (RNP) assembly involved in translational silencing or RNA degradation. Yet, the dynamics of RNP assembly and its underlying functional implications are unknown. Here, we have characterized the role of the RNA-binding protein Staufen2, a candidate Ago interactor, in RNP assembly. Staufen2 depletion resulted in the upregulation of Ago1/2 and the RISC effector proteins Ddx6 and Dcp1a. This upregulation was accompanied by the displacement of Ago1/2 from processing bodies, large RNPs implicated in RNA storage, and subsequent association of Ago2 with polysomes. In parallel, Staufen2 deficiency decreased global translation and increased dendritic branching. As the observed phenotypes can be rescued by Ago1/2 knockdown, we propose a working model in which both Staufen2 and Ago proteins depend on each other and contribute to neuronal homeostasis.

摘要

成熟的 microRNAs 与 Argonaute(Ago1-4)蛋白家族的成员结合,形成 RNA 诱导沉默复合物(RISC)的核心。RISC 与靶 mRNA 的结合导致参与翻译沉默或 RNA 降解的核糖核蛋白(RNP)组装。然而,RNP 组装的动力学及其潜在的功能意义尚不清楚。在这里,我们描述了 RNA 结合蛋白 Staufen2(Ago 相互作用的候选蛋白)在 RNP 组装中的作用。Staufen2 耗竭导致 Ago1/2 和 RISC 效应蛋白 Ddx6 和 Dcp1a 的上调。这种上调伴随着 Ago1/2 从参与 RNA 储存的大核糖核蛋白(processing bodies)中的位移,以及随后 Ago2 与多核糖体的结合。与此同时,Staufen2 缺乏会降低全局翻译并增加树突分支。由于观察到的表型可以通过 Ago1/2 的敲低挽救,我们提出了一个工作模型,其中 Staufen2 和 Ago 蛋白相互依赖,并有助于神经元的内稳态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/559c/9262589/80c37edc9749/gkac487fig1.jpg

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