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白色念珠菌质膜胞膜窖蛋白的邻近标记鉴定

Proximity labeling identification of plasma membrane eisosome proteins in Candida albicans.

作者信息

Lanze Carla E, Haley John D, Konopka James B

机构信息

Department of Microbiology and Immunology, Renaissance School of Medicine, Stony Brook University, Stony Brook, NY 11794, USA.

Department of Pathology, Renaissance School of Medicine, Stony Brook University, Stony Brook, NY 11794, USA.

出版信息

Genetics. 2025 Apr 28. doi: 10.1093/genetics/iyaf077.

DOI:10.1093/genetics/iyaf077
PMID:40294162
Abstract

The ability of Candida albicans to resist stressful conditions in the host and grow invasively into tissues contributes to the virulence of this human fungal pathogen. Plasma membrane subdomains known as the MCC (Membrane Compartment of Can1) or eisosomes are important for these processes. MCC/eisosome domains are furrow-shaped invaginations of the plasma membrane that are about 250 nm long and 50 nm deep. To identify proteins that localize to these domains, a proximity labeling method was used in which the TurboID variant of the BirA biotin ligase was fused to Sur7 and Lsp1, two proteins that localize to eisosomes and are important for virulence. This resulted in biotinylation of nearby proteins, permitting their identification. Analysis of 19 candidate proteins by tagging with the Green Fluorescent Protein (GFP) identified 7 proteins that detectably overlapped with MCC/eisosomes. Deletion mutant analysis showed that one of these, a poorly studied protein known as Ker1, was important for hyphal growth in liquid culture, invasive growth into agar medium, and resistance to stress caused by copper and cell wall perturbing agents. Altogether, these approaches identified novel MCC/eisosome proteins and show that TurboID can be applied to better define the molecular mechanisms of C. albicans pathogenesis and aid in discovery of targets for novel therapeutic strategies.

摘要

白色念珠菌抵抗宿主体内应激条件并侵入组织生长的能力,促成了这种人类真菌病原体的毒力。被称为MCC(Can1膜区室)或胞膜窖的质膜亚结构域对这些过程很重要。MCC/胞膜窖结构域是质膜上的沟状内陷,长约250纳米,深约50纳米。为了鉴定定位于这些结构域的蛋白质,使用了一种邻近标记方法,即将BirA生物素连接酶的TurboID变体与Sur7和Lsp1融合,这两种蛋白质定位于胞膜窖且对毒力很重要。这导致附近蛋白质的生物素化,从而便于对其进行鉴定。通过用绿色荧光蛋白(GFP)标记对19种候选蛋白质进行分析,鉴定出7种与MCC/胞膜窖可检测到重叠的蛋白质。缺失突变体分析表明,其中一种研究较少的蛋白质Ker1,对液体培养中的菌丝生长、侵入琼脂培养基生长以及对铜和细胞壁干扰剂引起的应激的抗性很重要。总之,这些方法鉴定出了新的MCC/胞膜窖蛋白质,并表明TurboID可用于更好地定义白色念珠菌致病的分子机制,并有助于发现新治疗策略的靶点。

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Proximity labeling identification of plasma membrane eisosome proteins in Candida albicans.白色念珠菌质膜胞膜窖蛋白的邻近标记鉴定
Genetics. 2025 Apr 28. doi: 10.1093/genetics/iyaf077.
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本文引用的文献

1
The Candida Genome Database: annotation and visualization updates.念珠菌基因组数据库:注释与可视化更新
Genetics. 2025 Mar 17;229(3). doi: 10.1093/genetics/iyaf001.
2
The Cwr1 protein kinase localizes to the plasma membrane and mediates resistance to cell wall stress in .Cwr1蛋白激酶定位于质膜,并介导对细胞壁应激的抗性。
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Characterization of BioID tagging systems in budding yeast and exploring the interactome of the Ccr4-Not complex.
酵母中 BioID 标记系统的特征分析及 Ccr4-Not 复合物互作组的探索。
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Sur7 mediates a novel pathway for PIP regulation in that promotes stress resistance and cell wall morphogenesis.Sur7 介导了一个在 中调控 PIP 的新途径,该途径促进了应激抗性和细胞壁形态发生。
Mol Biol Cell. 2024 Jul 1;35(7):ar99. doi: 10.1091/mbc.E23-08-0324. Epub 2024 May 22.
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The WHO fungal priority pathogens list: a crucial reappraisal to review the prioritisation.世界卫生组织真菌优先病原体清单:重新评估以审查优先级的关键
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Ferroptosis-protective membrane domains in quiescence.静止期具有铁死亡防护作用的膜结构域。
Cell Rep. 2023 Dec 26;42(12):113561. doi: 10.1016/j.celrep.2023.113561. Epub 2023 Dec 12.
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Tetraspanner-based nanodomains modulate BAR domain-induced membrane curvature.基于 Tetraspanner 的纳米域调节 BAR 结构域诱导的膜曲率。
EMBO Rep. 2023 Dec 6;24(12):e57232. doi: 10.15252/embr.202357232. Epub 2023 Oct 30.
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The Ypk1 protein kinase signaling pathway is rewired and not essential for viability in Candida albicans.Ypk1 蛋白激酶信号通路在白念珠菌中被重新布线,对于其生存并非必需。
PLoS Genet. 2023 Aug 10;19(8):e1010890. doi: 10.1371/journal.pgen.1010890. eCollection 2023 Aug.
10
Recent advances in membrane mimetics for membrane protein research.近年来用于膜蛋白研究的膜模拟物的进展。
Biochem Soc Trans. 2023 Jun 28;51(3):1405-1416. doi: 10.1042/BST20230164.