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Sharpin 相互作用组揭示了 Sharpin 通过 Arp2/3 复合物在片状伪足形成中的作用。

The Sharpin interactome reveals a role for Sharpin in lamellipodium formation via the Arp2/3 complex.

机构信息

Turku Centre for Biotechnology, University of Turku and Åbo Akademi University, Turku 20520, Finland.

Turku Doctoral Programme of Molecular Medicine, University of Turku, Turku 20520, Finland.

出版信息

J Cell Sci. 2017 Sep 15;130(18):3094-3107. doi: 10.1242/jcs.200329. Epub 2017 Aug 3.

Abstract

Sharpin, a multifunctional adaptor protein, regulates several signalling pathways. For example, Sharpin enhances signal-induced NF-κB signalling as part of the linear ubiquitin assembly complex (LUBAC) and inhibits integrins, the T cell receptor, caspase 1 and PTEN. However, despite recent insights into Sharpin and LUBAC function, a systematic approach to identify the signalling pathways regulated by Sharpin has not been reported. Here, we present the first 'Sharpin interactome', which identifies a large number of novel potential Sharpin interactors in addition to several known ones. These data suggest that Sharpin and LUBAC might regulate a larger number of biological processes than previously identified, such as endosomal trafficking, RNA processing, metabolism and cytoskeleton regulation. Importantly, using the Sharpin interactome, we have identified a novel role for Sharpin in lamellipodium formation. We demonstrate that Sharpin interacts with Arp2/3, a protein complex that catalyses actin filament branching. We have identified the Arp2/3-binding site in Sharpin and demonstrate using a specific Arp2/3-binding deficient mutant that the Sharpin-Arp2/3 interaction promotes lamellipodium formation in a LUBAC-independent fashion.This article has an associated First Person interview with the first author of the paper.

摘要

Shapin 是一种多功能衔接蛋白,可调节多种信号通路。例如,Shapin 增强信号诱导的 NF-κB 信号通路,作为线性泛素组装复合物 (LUBAC) 的一部分,并抑制整合素、T 细胞受体、半胱天冬酶 1 和 PTEN。然而,尽管最近对 Shapin 和 LUBAC 的功能有了深入了解,但尚未有系统的方法来鉴定 Shapin 调节的信号通路。在这里,我们首次展示了“Shapin 相互作用组”,除了几个已知的相互作用蛋白外,还鉴定了大量新的潜在 Shapin 相互作用蛋白。这些数据表明,Shapin 和 LUBAC 可能调节比以前发现的更多的生物学过程,如内体运输、RNA 处理、代谢和细胞骨架调节。重要的是,我们利用 Shapin 相互作用组,鉴定了 Shapin 在片状伪足形成中的一个新作用。我们证明 Shapin 与 Arp2/3 相互作用,Arp2/3 是一种催化肌动蛋白丝分支的蛋白质复合物。我们确定了 Shapin 中的 Arp2/3 结合位点,并通过特定的 Arp2/3 结合缺陷突变体证明,Shapin-Arp2/3 相互作用以 LUBAC 非依赖性的方式促进片状伪足的形成。本文有该论文第一作者的相关第一人称采访。

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