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白色念珠菌的PEP12对于生物膜完整性和体内毒力是必需的。

Candida albicans PEP12 is required for biofilm integrity and in vivo virulence.

作者信息

Palanisamy Suresh K A, Ramirez Melissa A, Lorenz Michael, Lee Samuel A

机构信息

Division of Infectious Diseases, New Mexico Veterans Healthcare System, Albuquerque, NM 87108, USA.

出版信息

Eukaryot Cell. 2010 Feb;9(2):266-77. doi: 10.1128/EC.00295-09. Epub 2009 Dec 18.

Abstract

To investigate the role of the prevacuolar secretion pathway in biofilm formation and virulence in Candida albicans, we cloned and analyzed the C. albicans homolog of the Saccharomyces cerevisiae prevacuolar trafficking gene PEP12. C. albicans PEP12 encodes a deduced t-SNARE that is 28% identical to S. cerevisiae Pep12p, and plasmids bearing C. albicans PEP12 complemented the abnormal vacuolar morphology and temperature-sensitive growth of an S. cerevisiae pep12 null mutant. The C. albicans pep12 Delta null mutant was defective in endocytosis and vacuolar acidification and accumulated 40- to 60-nm cytoplasmic vesicles near the plasma membrane. Secretory defects included increased extracellular proteolytic activity and absent lipolytic activity. The pep12Delta null mutant was more sensitive to cell wall stresses and antifungal agents than the isogenic complemented strain or the control strain DAY185. Notably, the biofilm formed by the pep12Delta mutant was reduced in overall mass and fragmented completely upon the slightest disturbance. The pep12Delta mutant was markedly reduced in virulence in an in vitro macrophage infection model and an in vivo mouse model of disseminated candidiasis. These results suggest that C. albicans PEP12 plays a key role in biofilm integrity and in vivo virulence.

摘要

为了研究液泡前分泌途径在白色念珠菌生物膜形成和毒力中的作用,我们克隆并分析了酿酒酵母液泡前运输基因PEP12的白色念珠菌同源物。白色念珠菌PEP12编码一种推导的t-SNARE,与酿酒酵母Pep12p有28%的同一性,携带白色念珠菌PEP12的质粒补充了酿酒酵母pep12缺失突变体的异常液泡形态和温度敏感生长。白色念珠菌pep12Δ缺失突变体在胞吞作用和液泡酸化方面存在缺陷,并在质膜附近积累了40至60纳米的细胞质囊泡。分泌缺陷包括细胞外蛋白水解活性增加和脂肪分解活性缺失。pep12Δ缺失突变体比同基因互补菌株或对照菌株DAY185对细胞壁应激和抗真菌剂更敏感。值得注意的是,pep12Δ突变体形成的生物膜总质量减少,在最轻微的干扰下就会完全破碎。在体外巨噬细胞感染模型和体内播散性念珠菌病小鼠模型中,pep12Δ突变体的毒力明显降低。这些结果表明,白色念珠菌PEP12在生物膜完整性和体内毒力中起关键作用。

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