Impact of secreted glucanases upon the cell surface and fitness of Candida albicans during colonisation and infection

Q1 Immunology and Microbiology Cell Surface Pub Date : 2024-06-01 DOI:10.1016/j.tcsw.2024.100128
Qinxi Ma , Arnab Pradhan , Ian Leaves , Emer Hickey , Elena Roselletti , Ivy Dambuza , Daniel E. Larcombe , Leandro Jose de Assis , Duncan Wilson , Lars P. Erwig , Mihai G. Netea , Delma S. Childers , Gordon D. Brown , Neil A.R. Gow , Alistair J.P. Brown
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Abstract

Host recognition of the pathogen-associated molecular pattern (PAMP), β-1,3-glucan, plays a major role in antifungal immunity. β-1,3-glucan is an essential component of the inner cell wall of the opportunistic pathogen Candida albicans. Most β-1,3-glucan is shielded by the outer cell wall layer of mannan fibrils, but some can become exposed at the cell surface. In response to host signals such as lactate, C. albicans shaves the exposed β-1,3-glucan from its cell surface, thereby reducing the ability of innate immune cells to recognise and kill the fungus. We have used sets of barcoded xog1 and eng1 mutants to compare the impacts of the secreted β-glucanases Xog1 and Eng1 upon C. albicans in vitro and in vivo. Flow cytometry of Fc-dectin-1-stained strains revealed that Eng1 plays the greater role in lactate-induced β-1,3-glucan masking. Transmission electron microscopy and stress assays showed that neither Eng1 nor Xog1 are essential for cell wall maintenance, but the inactivation of either enzyme compromised fungal adhesion to gut and vaginal epithelial cells. Competitive barcode sequencing suggested that neither Eng1 nor Xog1 strongly influence C. albicans fitness during systemic infection or vaginal colonisation in mice. However, the deletion of XOG1 enhanced C. albicans fitness during gut colonisation. We conclude that both Eng1 and Xog1 exert subtle effects on the C. albicans cell surface that influence fungal adhesion to host cells and that affect fungal colonisation in certain host niches.

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在定植和感染过程中,分泌葡聚糖酶对白色念珠菌细胞表面和适应性的影响
宿主对病原体相关分子模式(PAMP)β-1,3-葡聚糖的识别在抗真菌免疫中发挥着重要作用。β-1,3-葡聚糖是机会性病原体白色念珠菌内细胞壁的重要组成部分。大部分 β-1,3-葡聚糖被细胞外壁的甘露聚糖纤维层所保护,但也有一部分暴露在细胞表面。为了对乳酸等宿主信号做出反应,白念珠菌会将暴露的 β-1,3-葡聚糖从细胞表面刮掉,从而降低先天性免疫细胞识别和杀死真菌的能力。我们利用一组条形码 Xog1 和 Eng1 突变体,比较了分泌型 β-葡聚糖酶 Xog1 和 Eng1 在体外和体内对白僵菌的影响。Fc-Dectin-1染色菌株的流式细胞仪显示,Eng1在乳酸盐诱导的β-1,3-葡聚糖掩蔽中发挥了更大的作用。透射电子显微镜和压力试验表明,Eng1 和 Xog1 对细胞壁的维持都不是必需的,但这两种酶的失活都会影响真菌对肠道和阴道上皮细胞的粘附。竞争性条形码测序表明,在小鼠全身感染或阴道定植过程中,Eng1 和 Xog1 都不会对白僵菌的适应性产生强烈影响。然而,删除 XOG1 会增强白僵菌在肠道定植过程中的适应性。我们的结论是,Eng1 和 Xog1 对白僵菌细胞表面都有微妙的影响,它们影响真菌对宿主细胞的粘附,并影响真菌在某些宿主壁龛中的定殖。
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来源期刊
Cell Surface
Cell Surface Immunology and Microbiology-Applied Microbiology and Biotechnology
CiteScore
6.10
自引率
0.00%
发文量
18
审稿时长
49 days
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