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2
Interaction of yeast Rvs167 and Pho85 cyclin-dependent kinase complexes may link the cell cycle to the actin cytoskeleton.酵母Rvs167与Pho85细胞周期蛋白依赖性激酶复合物之间的相互作用可能将细胞周期与肌动蛋白细胞骨架联系起来。
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The WASp homologue Las17p functions with the WIP homologue End5p/verprolin and is essential for endocytosis in yeast.WASp 同源物 Las17p 与 WIP 同源物 End5p/肌动蛋白结合蛋白协同发挥作用,对酵母的内吞作用至关重要。
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The Src homology domain 3 (SH3) of a yeast type I myosin, Myo5p, binds to verprolin and is required for targeting to sites of actin polarization.酵母I型肌球蛋白Myo5p的Src同源结构域3(SH3)与维普洛林结合,是靶向肌动蛋白极化位点所必需的。
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Cyclin partners determine Pho85 protein kinase substrate specificity in vitro and in vivo: control of glycogen biosynthesis by Pcl8 and Pcl10.细胞周期蛋白伴侣在体外和体内决定Pho85蛋白激酶的底物特异性:Pcl8和Pcl10对糖原生物合成的调控
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10
Rvs161p interacts with Fus2p to promote cell fusion in Saccharomyces cerevisiae.Rvs161p与Fus2p相互作用,以促进酿酒酵母中的细胞融合。
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酵母Rvs167p结构域的体内分析表明,Rvs167p的功能是通过多种蛋白质相互作用介导的。

In vivo analysis of the domains of yeast Rvs167p suggests Rvs167p function is mediated through multiple protein interactions.

作者信息

Colwill K, Field D, Moore L, Friesen J, Andrews B

机构信息

Department of Molecular and Medical Genetics, University of Toronto, Toronto, Ontario M5S 1A8, Canada.

出版信息

Genetics. 1999 Jul;152(3):881-93. doi: 10.1093/genetics/152.3.881.

DOI:10.1093/genetics/152.3.881
PMID:10388809
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1460664/
Abstract

Morphological changes during cell division in the yeast Saccharomyces cerevisiae are controlled by cell-cycle regulators. The Pcl-Pho85p kinase complex has been implicated in the regulation of the actin cytoskeleton at least in part through Rvs167p. Rvs167p consists of three domains called BAR, GPA, and SH3. Using a two-hybrid assay, we demonstrated that each region of Rvs167p participates in protein-protein interactions: the BAR domain bound the BAR domain of another Rvs167p protein and that of Rvs161p, the GPA region bound Pcl2p, and the SH3 domain bound Abp1p. We identified Rvs167p as a Las17p/Bee1p-interacting protein in a two-hybrid screen and showed that Las17p/Bee1p bound the SH3 domain of Rvs167p. We tested the extent to which the Rvs167p protein domains rescued phenotypes associated with deletion of RVS167: salt sensitivity, random budding, and endocytosis and sporulation defects. The BAR domain was sufficient for full or partial rescue of all rvs167 mutant phenotypes tested but not required for the sporulation defect for which the SH3 domain was also sufficient. Overexpression of Rvs167p inhibits cell growth. The BAR domain was essential for this inhibition and the SH3 domain had only a minor effect. Rvs167p may link the cell cycle regulator Pcl-Pho85p kinase and the actin cytoskeleton. We propose that Rvs167p is activated by phosphorylation in its GPA region by the Pcl-Pho85p kinase. Upon activation, Rvs167p enters a multiprotein complex, making critical contacts in its BAR domain and redundant or minor contacts with its SH3 domain.

摘要

酿酒酵母细胞分裂过程中的形态变化受细胞周期调节因子控制。Pcl-Pho85p激酶复合体至少部分通过Rvs167p参与肌动蛋白细胞骨架的调节。Rvs167p由称为BAR、GPA和SH3的三个结构域组成。通过双杂交试验,我们证明Rvs167p的每个区域都参与蛋白质-蛋白质相互作用:BAR结构域与另一个Rvs167p蛋白的BAR结构域以及Rvs161p的BAR结构域结合,GPA区域与Pcl2p结合,SH3结构域与Abp1p结合。我们在双杂交筛选中鉴定出Rvs167p是一种与Las17p/Bee1p相互作用的蛋白,并表明Las17p/Bee1p与Rvs167p的SH3结构域结合。我们测试了Rvs167p蛋白结构域挽救与RVS167缺失相关表型的程度:盐敏感性、随机出芽、内吞作用以及孢子形成缺陷。BAR结构域足以完全或部分挽救所测试的所有rvs167突变体表型,但对于孢子形成缺陷不是必需的,SH3结构域对此也足够。Rvs167p的过表达抑制细胞生长。BAR结构域对于这种抑制至关重要,而SH3结构域只有轻微影响。Rvs167p可能连接细胞周期调节因子Pcl-Pho85p激酶和肌动蛋白细胞骨架。我们提出Rvs167p在其GPA区域被Pcl-Pho85p激酶磷酸化而激活。激活后,Rvs167p进入一个多蛋白复合体,在其BAR结构域形成关键接触,并与其SH3结构域形成冗余或次要接触。