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白念珠菌中的 Pga13 定位于细胞壁,影响细胞表面特性、形态发生和毒力。

Pga13 in Candida albicans is localized in the cell wall and influences cell surface properties, morphogenesis and virulence.

机构信息

GMCA Research Unit, Departamento de Microbiología y Ecología, Universidad de Valencia, E-46100 Burjassot, Valencia, Spain.

出版信息

Fungal Genet Biol. 2012 Apr;49(4):322-31. doi: 10.1016/j.fgb.2012.01.010. Epub 2012 Feb 8.

DOI:10.1016/j.fgb.2012.01.010
PMID:22343036
Abstract

The fungal cell wall is an essential organelle required for maintaining cell integrity and also plays an important role in the primary interactions between pathogenic fungi and their hosts. PGA13 encodes a GPI protein in the human pathogen Candida albicans, which is highly up-regulated during cell wall regeneration in protoplasts. The Pga13 protein contains a unique tandem repeat, which is present five times and is characterized by conserved spacing between the four cysteine residues. Furthermore, the mature protein contains 38% serine and threonine residues, and therefore probably is a highly glycosylated cell wall protein. Consistent with this, a chimeric Pga13-V5 protein could be localized to the cell wall, but only after deglycosylation was performed. Disruption of PGA13 led to increased sensitivity to Congo red, Calcofluor white, and zymolyase, and to a diminished ability of protoplasts to recover their cell wall. In addition, pga13Δ mutants exhibited delayed filamentation, a higher surface hydrophobicity, and increased adherence and flocculation (cell-cell interactions). Furthermore, transcript profiling showed that expression of four members of the ALS family (adhesin-encoding genes) is up-regulated in the pga13Δ null mutant. Altogether, these results indicate that Pga13 is a wall-localized protein that contributes to cell wall synthesis and is important for acquiring normal surface properties. The contribution of Pga13 to surface hydrophilicity may be important for cell dispersal during development of invasive infections, and possibly for morphological development. This is consistent with the observed reduced virulence of pga13Δ mutants in a mouse model of disseminated candidiasis.

摘要

真菌细胞壁是维持细胞完整性所必需的细胞器,在病原真菌与其宿主之间的初始相互作用中也起着重要作用。PGA13 编码人类病原体白色念珠菌中的一种 GPI 蛋白,该蛋白在原生质体细胞壁再生过程中高度上调。Pga13 蛋白含有独特的串联重复序列,该序列出现五次,并且四个半胱氨酸残基之间的间隔保守。此外,成熟蛋白含有 38%的丝氨酸和苏氨酸残基,因此可能是一种高度糖基化的细胞壁蛋白。与这一观点一致的是,嵌合 Pga13-V5 蛋白可以定位于细胞壁,但只有在进行去糖基化后才能定位。PGA13 的缺失导致对刚果红、Calcofluor white 和几丁质酶的敏感性增加,以及原生质体恢复细胞壁的能力减弱。此外,pga13Δ突变体表现出丝状生长延迟、更高的表面疏水性、增加的粘附和絮凝(细胞-细胞相互作用)。此外,转录谱分析表明,ALS 家族(粘附素编码基因)的四个成员的表达在 pga13Δ 缺失突变体中上调。总的来说,这些结果表明 Pga13 是一种定位于细胞壁的蛋白,有助于细胞壁合成,对于获得正常的表面特性很重要。Pga13 对表面亲水性的贡献可能对侵袭性感染发展过程中细胞的分散很重要,并且可能对形态发育也很重要。这与 pga13Δ 突变体在播散性念珠菌病的小鼠模型中观察到的毒力降低一致。

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