Function and Regulation of Cph2 in Candida albicans.

Eukaryotic Cell Pub Date : 2015-11-01 Epub Date: 2015-09-04 DOI:10.1128/EC.00102-15
Shelley Lane, Pietro Di Lena, Kati Tormanen, Pierre Baldi, Haoping Liu
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引用次数: 20

Abstract

Candida albicans is associated with humans as both a harmless commensal organism and a pathogen. Cph2 is a transcription factor whose DNA binding domain is similar to that of mammalian sterol response element binding proteins (SREBPs). SREBPs are master regulators of cellular cholesterol levels and are highly conserved from fungi to mammals. However, ergosterol biosynthesis is regulated by the zinc finger transcription factor Upc2 in C. albicans and several other yeasts. Cph2 is not necessary for ergosterol biosynthesis but is important for colonization in the murine gastrointestinal (GI) tract. Here we demonstrate that Cph2 is a membrane-associated transcription factor that is processed to release the N-terminal DNA binding domain like SREBPs, but its cleavage is not regulated by cellular levels of ergosterol or oxygen. Chromatin immunoprecipitation sequencing (ChIP-seq) shows that Cph2 binds to the promoters of HMS1 and other components of the regulatory circuit for GI tract colonization. In addition, 50% of Cph2 targets are also bound by Hms1 and other factors of the regulatory circuit. Several common targets function at the head of the glycolysis pathway. Thus, Cph2 is an integral part of the regulatory circuit for GI colonization that regulates glycolytic flux. Transcriptome sequencing (RNA-seq) shows a significant overlap in genes differentially regulated by Cph2 and hypoxia, and Cph2 is important for optimal expression of some hypoxia-responsive genes in glycolysis and the citric acid cycle. We suggest that Cph2 and Upc2 regulate hypoxia-responsive expression in different pathways, consistent with a synthetic lethal defect of the cph2 upc2 double mutant in hypoxia.

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Cph2在白色念珠菌中的作用及调控。
白色念珠菌作为一种无害的共生生物和病原体与人类有关。Cph2是一种DNA结合域与哺乳动物固醇反应元件结合蛋白(SREBPs)相似的转录因子。SREBPs是细胞胆固醇水平的主要调节因子,从真菌到哺乳动物都高度保守。然而,麦角甾醇的生物合成受锌指转录因子Upc2在白色念珠菌和其他几种酵母中的调节。Cph2不是麦角甾醇生物合成所必需的,但对小鼠胃肠道(GI)的定植很重要。在这里,我们证明了Cph2是一种膜相关转录因子,可以像SREBPs一样释放n端DNA结合域,但它的切割不受细胞麦角甾醇或氧水平的调节。染色质免疫沉淀测序(ChIP-seq)显示,Cph2结合HMS1的启动子和胃肠道定植调控回路的其他组分。此外,50%的Cph2靶点还受到Hms1等调控回路因子的约束。几个常见的靶点在糖酵解途径的头部起作用。因此,Cph2是调节糖酵解通量的胃肠道定殖调控回路的一个组成部分。转录组测序(RNA-seq)显示,受Cph2和缺氧差异调控的基因存在显著重叠,Cph2对糖酵解和柠檬酸循环中一些缺氧反应基因的最佳表达至关重要。我们认为Cph2和Upc2通过不同的途径调节低氧反应表达,这与Cph2 Upc2双突变体在低氧条件下的合成致死缺陷一致。
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来源期刊
Eukaryotic Cell
Eukaryotic Cell 生物-微生物学
自引率
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审稿时长
1 months
期刊介绍: Eukaryotic Cell (EC) focuses on eukaryotic microbiology and presents reports of basic research on simple eukaryotic microorganisms, such as yeasts, fungi, algae, protozoa, and social amoebae. The journal also covers viruses of these organisms and their organelles and their interactions with other living systems, where the focus is on the eukaryotic cell. Topics include: - Basic biology - Molecular and cellular biology - Mechanisms, and control, of developmental pathways - Structure and form inherent in basic biological processes - Cellular architecture - Metabolic physiology - Comparative genomics, biochemistry, and evolution - Population dynamics - Ecology
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