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单萜香芹酚在致病性真菌白色念珠菌中引发内质网应激。

The Monoterpene Carvacrol Generates Endoplasmic Reticulum Stress in the Pathogenic Fungus Candida albicans.

作者信息

Chaillot Julien, Tebbji Faiza, Remmal Adnane, Boone Charlie, Brown Grant W, Bellaoui Mohammed, Sellam Adnane

机构信息

Infectious Diseases Research Centre (CRI), CHU de Québec Research Center (CHUQ), Université Laval, Quebec City, Quebec, Canada.

Laboratoire de Biotechnologie, Faculty of Science of Fes, Sidi Mohammed Ben Abdallah University, Atlas Fes, Morocco.

出版信息

Antimicrob Agents Chemother. 2015 Aug;59(8):4584-92. doi: 10.1128/AAC.00551-15. Epub 2015 May 26.

Abstract

The monoterpene carvacrol, the major component of oregano and thyme oils, is known to exert potent antifungal activity against the pathogenic yeast Candida albicans. This monoterpene has been the subject of a considerable number of investigations that uncovered extensive pharmacological properties, including antifungal and antibacterial effects. However, its mechanism of action remains elusive. Here, we used integrative chemogenomic approaches, including genome-scale chemical-genetic and transcriptional profiling, to uncover the mechanism of action of carvacrol associated with its antifungal property. Our results clearly demonstrated that fungal cells require the unfolded protein response (UPR) signaling pathway to resist carvacrol. The mutants most sensitive to carvacrol in our genome-wide competitive fitness assay in the yeast Saccharomyces cerevisiae expressed mutations of the transcription factor Hac1 and the endonuclease Ire1, which is required for Hac1 activation by removing a nonconventional intron from the 3' region of HAC1 mRNA. Confocal fluorescence live-cell imaging revealed that carvacrol affects the morphology and the integrity of the endoplasmic reticulum (ER). Transcriptional profiling of pathogenic yeast C. albicans cells treated with carvacrol demonstrated a bona fide UPR transcriptional signature. Ire1 activity detected by the splicing of HAC1 mRNA in C. albicans was activated by carvacrol. Furthermore, carvacrol was found to potentiate antifungal activity of the echinocandin antifungal caspofungin and UPR inducers dithiothreitol and tunicamycin against C. albicans. This comprehensive chemogenomic investigation demonstrated that carvacrol exerts its antifungal activity by altering ER integrity, leading to ER stress and the activation of the UPR to restore protein-folding homeostasis.

摘要

香芹酚是牛至油和百里香油的主要成分,已知其对致病性酵母白色念珠菌具有强大的抗真菌活性。这种单萜类化合物一直是大量研究的主题,这些研究揭示了其广泛的药理特性,包括抗真菌和抗菌作用。然而,其作用机制仍然不明。在此,我们使用了整合化学基因组学方法,包括全基因组化学遗传和转录谱分析,以揭示香芹酚与其抗真菌特性相关的作用机制。我们的结果清楚地表明,真菌细胞需要未折叠蛋白反应(UPR)信号通路来抵抗香芹酚。在我们对酿酒酵母进行的全基因组竞争适应性测定中,对香芹酚最敏感的突变体表达了转录因子Hac1和核酸内切酶Ire1的突变,Ire1通过从HAC1 mRNA的3'区域去除一个非常规内含子来激活Hac1。共聚焦荧光活细胞成像显示,香芹酚会影响内质网(ER)的形态和完整性。用香芹酚处理致病性酵母白色念珠菌细胞的转录谱分析显示出真正的UPR转录特征。通过白色念珠菌中HAC1 mRNA的剪接检测到的Ire1活性被香芹酚激活。此外,发现香芹酚可增强棘白菌素类抗真菌药物卡泊芬净以及UPR诱导剂二硫苏糖醇和衣霉素对白色念珠菌的抗真菌活性。这项全面的化学基因组学研究表明,香芹酚通过改变内质网完整性发挥其抗真菌活性,导致内质网应激并激活UPR以恢复蛋白质折叠稳态。

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