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首页> 外文期刊>Eukaryotic cell >The Casein Kinase I Protein Cck1 Regulates Multiple Signaling Pathways and Is Essential for Cell Integrity and Fungal Virulence in Cryptococcus neoformans
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The Casein Kinase I Protein Cck1 Regulates Multiple Signaling Pathways and Is Essential for Cell Integrity and Fungal Virulence in Cryptococcus neoformans

机译:酪蛋白激酶I蛋白Cck1调节多种信号通路,对于新隐球菌的细胞完整性和真菌毒力必不可少

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摘要

Casein kinases regulate a wide range of cellular functions in eukaryotes, including phosphorylation of proteins that are substrates for degradation via the ubiquitin-proteasome system (UPS). Our previous study demonstrated that Fbp1, a component of the SCFFBP1 E3 ligase complex, was essential for Cryptococcus virulence. Because the Saccharomyces cerevisiae homolog of Fbp1, Grr1, requires casein kinase I (Yck1 and Yck2) to phosphorylate its substrates, we investigated the function of casein kinase I in Cryptococcus neoformans. In this report, we identified a C. neoformans casein kinase I protein homolog, Cck1. Similar to Fbp1, the expression of Cck1 is negatively regulated by glucose and during mating. cck1 null mutants showed significant virulence attenuation in a murine systemic infection model, but Cck1 was dispensable for the development of classical virulence factors (capsule, melanin, and growth at 37°C). cck1 mutants were hypersensitive to SDS treatment, indicating that Cck1 is required for cell integrity. The functional overlap between Cck1 and Fbp1 suggests that Cck1 may be required for the phosphorylation of Fbp1 substrates. Interestingly, the cck1 mutant also showed increased sensitivity to osmotic stress and oxidative stress, suggesting that Cck1 regulates both cell integrity and the cellular stress response. Our results show that Cck1 regulates the phosphorylation of both Mpk1 and Hog1 mitogen-activated protein kinases (MAPKs), demonstrating that Cck1 regulates cell integrity via the Mpk1 pathway and regulates cell adaptation to stresses via the Hog1 pathway. Overall, our study revealed that Cck1 plays important roles in regulating multiple signaling pathways and is required for fungal pathogenicity.
机译:酪蛋白激酶调节真核生物中广泛的细胞功能,包括蛋白质的磷酸化,蛋白质是通过泛素-蛋白酶体系统(UPS)降解的底物。我们以前的研究表明,Fbp1是SCF FBP1 E3连接酶复合物的组成部分,对于隐球菌毒力至关重要。由于Fbp1,Grr1的酿酒酵母同源物需要酪蛋白激酶I(Yck1和Yck2)磷酸化其底物,因此我们研究了酪蛋白激酶I在新型隐球菌中的功能。在此报告中,我们鉴定了新孢梭菌酪蛋白激酶I蛋白同源物Cck1。类似于Fbp1,Cck1的表达受到葡萄糖和交配的负调控。 cck1 无效突变体在小鼠全身感染模型中显示出显着的毒力减弱,但是Cck1对于经典毒力因子(胶囊,黑色素和37°C的生长)的发展是不可或缺的。 cck1 突变体对SDS处理非常敏感,表明Cck1是细胞完整性所必需的。 Cck1和Fbp1之间的功能重叠表明Fck1底物的磷酸化可能需要Cck1。有趣的是, cck1 突变体还显示出对渗透压和氧化应激的敏感性增加,表明Cck1调节细胞完整性和细胞应激反应。我们的结果表明,Cck1调节Mpk1和Hog1丝裂原活化蛋白激酶(MAPKs)的磷酸化,表明Cck1通过Mpk1途径调节细胞完整性,并通过Hog1途径调节细胞对应激的适应性。总体而言,我们的研究表明Cck1在调节多种信号通路中起重要作用,并且是真菌致病性所必需的。

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