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Role for the SCFCDC4 Ubiquitin Ligase in Candida albicans Morphogenesis

机译:SCFCDC4泛素连接酶在白色念珠菌形态发生中的作用

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摘要

The ability of Candida albicans, a major fungal pathogen, to switch between a yeast form, and a hyphal (mold) form is recognized as being important for the ability of the organism to invade the host and cause disease. We found that a C. albicans mutant deleted for CaCDC4, a homologue of the Saccharomyces cerevisiae F-box protein component of the SCFCDC4 ubiquitin ligase, is viable and displays constitutive filamentous, mostly hyphal, growth. The phenotype of the Cacdc4–/– mutant suggests that ubiquitin-mediated protein degradation is involved in the regulation of the dimorphic switch of C. albicans and that one or more regulators of the yeast-to-mold switch are among the substrates of SCFCaCDC4. Epistasis analysis indicates that the Cacdc4–/– phenotype is largely independent of the filamentation-inducing transcription factors Efg1 and Cph1. We identify C. albicans Far1 and Sol1, homologues of the S. cerevisiae SCFCDC4 substrates Far1 and Sic1, and show that Sol1 is a substrate of C. albicans Cdc4. Neither protein is essential for the hyphal phenotype of the Cacdc4–/– mutant. However, ectopic expression and deletion of SOL1 indicate a role for this gene in C. albicans morphogenesis.
机译:主要的真菌病原体白色念珠菌在酵母形式和菌丝(霉菌)形式之间转换的能力被认为对生物入侵宿主并引起疾病的能力很重要。我们发现,缺失的白色念珠菌突变体CaCDC4(SCFCDC4泛素连接酶的酿酒酵母F-box蛋白成分的同源物)是可行的,并显示出组成性丝状(主要是菌丝状)生长。 Cacdc4 – / –突变体的表型表明,泛素介导的蛋白质降解参与了白色念珠菌的双态转换的调控,而酵母到霉菌转换的一个或多个调控子是SCFCaCDC4的底物。上位性分析表明,Cacdc4 – / –表型在很大程度上与诱导丝化的转录因子Efg1和Cph1无关。我们确定白色念珠菌Far1和Sol1,酿酒酵母SCFCDC4底物Far1和Sic1的同源物,并显示Sol1是白色念珠菌Cdc4的底物。 Cacdc4 – / –突变体的菌丝表型都不是必需的蛋白质。但是,异位表达和SOL1删除表明此基因在白色念珠菌形态发生中的作用。

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