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白色念珠菌中新型N-BAR异源二聚体Rvs162/Rvs167-3的鉴定与表征

Identification and characterization of Rvs162/Rvs167-3, a novel N-BAR heterodimer in the human fungal pathogen Candida albicans.

作者信息

Gkourtsa Areti, van den Burg Janny, Strijbis Karin, Avula Teja, Bijvoets Sietske, Timm Dave, Hochstenbach Frans, Distel Ben

机构信息

Department of Medical Biochemistry, Academic Medical Center, Amsterdam, The Netherlands.

Department of Infectious Diseases and Immunology, Utrecht University, Utrecht, The Netherlands.

出版信息

Eukaryot Cell. 2015 Feb;14(2):182-93. doi: 10.1128/EC.00282-14. Epub 2014 Dec 29.

Abstract

Membrane reshaping resides at the core of many important cellular processes, and among its mediators are the BAR (Bin, Amphiphysin, Rvs) domain-containing proteins. We have explored the diversity and function of the Rvs BAR proteins in Candida albicans and identified a novel family member, Rvs167-3 (orf19.1861). We show that Rvs167-3 specifically interacts with Rvs162 to form a stable BAR heterodimer able to bind liposomes in vitro. A second, distinct heterodimer is formed by the canonical BAR proteins Rvs161 and Rvs167. Purified Rvs161/Rvs167 complex also binds liposomes, indicating that C. albicans expresses two functional BAR heterodimers. We used live-cell imaging to localize green fluorescent protein (GFP)-tagged Rvs167-3 and Rvs167 and show that both proteins concentrate in small cortical spots. However, while Rvs167 strictly colocalizes with the endocytic marker protein Abp1, we do not observe any colocalization of Rvs167-3 with sites of endocytosis marked by Abp1. Furthermore, the rvs167-3Δ/Δ mutant is not defective in endocytosis and strains lacking Rvs167-3 or its partner Rvs162 do not display increased sensitivity to high salt concentrations or decreased cell wall integrity, phenotypes which have been observed for rvs167Δ/Δ and rvs161Δ/Δ strains and which are linked to endocytosis defects. Taken together, our results indicate different roles for the two BAR heterodimers in C. albicans: the canonical Rvs161/Rvs167 heterodimer functions in endocytosis, whereas the novel Rvs162/Rvs167-3 heterodimer seems not to be involved in this process. Nevertheless, despite their different roles, our phenotypic analysis revealed a genetic interaction between the two BAR heterodimers, suggesting that they may have related but distinct membrane-associated functions.

摘要

膜重塑是许多重要细胞过程的核心,其中介体包括含BAR(Bin、Amphiphysin、Rvs)结构域的蛋白质。我们探索了白色念珠菌中Rvs BAR蛋白的多样性和功能,并鉴定出一个新的家族成员Rvs167-3(orf19.1861)。我们发现Rvs167-3与Rvs162特异性相互作用,形成一个能够在体外结合脂质体的稳定BAR异二聚体。由经典BAR蛋白Rvs161和Rvs167形成了另一种不同的异二聚体。纯化的Rvs161/Rvs167复合物也能结合脂质体,这表明白色念珠菌表达两种功能性BAR异二聚体。我们使用活细胞成像技术对绿色荧光蛋白(GFP)标记的Rvs167-3和Rvs167进行定位,结果表明这两种蛋白都集中在小的皮质斑点中。然而,虽然Rvs167与内吞标记蛋白Abp1严格共定位,但我们未观察到Rvs167-3与由Abp1标记的内吞位点有任何共定位现象。此外,rvs167-3Δ/Δ突变体在内吞作用方面没有缺陷,缺乏Rvs167-3或其伙伴Rvs162的菌株对高盐浓度没有表现出增加的敏感性,细胞壁完整性也没有降低,而rvs167Δ/Δ和rvs161Δ/Δ菌株则出现了这些与内吞缺陷相关的表型。综上所述,我们的结果表明两种BAR异二聚体在白色念珠菌中发挥不同作用:经典的Rvs161/Rvs167异二聚体在内吞作用中起作用,而新的Rvs162/Rvs167-3异二聚体似乎不参与这一过程。然而,尽管它们作用不同,但我们的表型分析揭示了两种BAR异二聚体之间的遗传相互作用,这表明它们可能具有相关但不同的膜相关功能。

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