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Scar/WAVE 在细胞创伤修复过程中具有 Rac GTPase 非依赖性功能。

Scar/WAVE has Rac GTPase-independent functions during cell wound repair.

机构信息

Basic Sciences Division, Fred Hutchinson Cancer Center, 1100 Fairview Ave N, Seattle, WA, 98109, USA.

出版信息

Sci Rep. 2023 Mar 23;13(1):4763. doi: 10.1038/s41598-023-31973-2.

Abstract

Rho family GTPases regulate both linear and branched actin dynamics by activating downstream effectors to facilitate the assembly and function of complex cellular structures such as lamellipodia and contractile actomyosin rings. Wiskott-Aldrich Syndrome (WAS) family proteins are downstream effectors of Rho family GTPases that usually function in a one-to-one correspondence to regulate branched actin nucleation. In particular, the WAS protein Scar/WAVE has been shown to exhibit one-to-one correspondence with Rac GTPase. Here we show that Rac and SCAR are recruited to cell wounds in the Drosophila repair model and are required for the proper formation and maintenance of the dynamic actomyosin ring formed at the wound periphery. Interestingly, we find that SCAR is recruited to wounds earlier than Rac and is still recruited to the wound periphery in the presence of a potent Rac inhibitor. We also show that while Rac is important for actin recruitment to the actomyosin ring, SCAR serves to organize the actomyosin ring and facilitate its anchoring to the overlying plasma membrane. These differing spatiotemporal recruitment patterns and wound repair phenotypes highlight the Rac-independent functions of SCAR and provide an exciting new context in which to investigate these newly uncovered SCAR functions.

摘要

Rho 家族 GTPases 通过激活下游效应物来调节线性和分支肌动蛋白动力学,从而促进复杂细胞结构(如片状伪足和收缩性肌动球蛋白环)的组装和功能。Wiskott-Aldrich 综合征(WAS)家族蛋白是 Rho 家族 GTPases 的下游效应物,通常以一一对应的方式发挥作用,以调节分支肌动蛋白成核。特别是,WAS 蛋白 Scar/WAVE 已被证明与 Rac GTPase 呈一一对应关系。在这里,我们表明 Rac 和 SCAR 被招募到果蝇修复模型中的细胞伤口中,并且 Rac 和 SCAR 对于在伤口周围形成和维持动态肌动球蛋白环是必需的。有趣的是,我们发现 SCAR 比 Rac 更早地被招募到伤口,并且在存在有效的 Rac 抑制剂的情况下仍然被招募到伤口周围。我们还表明,虽然 Rac 对于肌动球蛋白环中肌动蛋白的募集很重要,但 SCAR 有助于组织肌动球蛋白环并促进其与上覆质膜的锚定。这些不同的时空招募模式和伤口修复表型突出了 SCAR 的 Rac 独立性功能,并为研究这些新发现的 SCAR 功能提供了一个令人兴奋的新背景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/df8e/10036328/300d9d64a6b9/41598_2023_31973_Fig1_HTML.jpg

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