The antifungal mechanism of EntV-derived peptides is associated with a reduction in extracellular vesicle release.

IF 4.9 1区 医学 Q1 MICROBIOLOGY
PLoS Pathogens Pub Date : 2025-09-22 eCollection Date: 2025-09-01 DOI:10.1371/journal.ppat.1013519
Giuseppe Buda De Cesare, Melissa R Cruz, Shane A Cristy, Luis A Vega, Robert Zarnowski, Antonino Zito, Shantanu Guha, David R Andes, Danielle A Garsin, Michael C Lorenz
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引用次数: 0

Abstract

Candida albicans, an opportunistic fungal pathogen, causes systemic and superficial infections, especially in immunocompromised patients. Treatment of fungal infections is complicated by limited antifungal options and the development of drug resistance. Previous work from our group demonstrated the efficacy of the anti-virulence peptide EntV and shorter variants against C. albicans infection in various animal models, including mouse models of oropharyngeal candidiasis and disseminated infection and a rat venous catheter model. However, the mechanism of action, which abrogates fungal virulence without fungicidal or fungistatic activity, has remained unknown. We used a combination of cell biological, biochemical, genomic, and genetic approaches to identify this mechanism. We demonstrate that EntV-based peptides bind to the fungal cell envelope in a punctate and dynamic manner, co-localizing with extracellular vesicles (EVs), which play a critical role in fungal biofilm formation and virulence. Transcriptomic and genetic analyses further indicate that this activity is linked to the intracellular vesicular trafficking machinery, especially the ESCRT pathway, as mutations in this pathway alter sensitivity to EntV peptides and regulate virulence. We also show that EntV treatment significantly reduces EV secretion in C. albicans, supporting a novel mechanism of antifungal action through inhibition of EV-mediated virulence. These findings further develop EntV as a promising anti-virulence agent with potential for therapeutic development against drug-resistant fungal pathogens.

entv衍生肽的抗真菌机制与细胞外囊泡释放的减少有关。
白色念珠菌是一种机会性真菌病原体,可引起全身和浅表感染,特别是在免疫功能低下的患者中。真菌感染的治疗由于有限的抗真菌药物选择和耐药性的发展而变得复杂。我们小组之前的工作在各种动物模型中证明了抗毒肽EntV和短变体对白色念珠菌感染的有效性,包括口咽念珠菌病和播散性感染的小鼠模型和大鼠静脉导管模型。然而,其作用机制,其消除真菌毒力而不杀真菌或抑真菌活性,仍然是未知的。我们结合细胞生物学、生物化学、基因组学和遗传学方法来确定这种机制。我们证明了基于entv的肽以点状和动态的方式与真菌细胞包膜结合,与细胞外囊泡(ev)共定位,后者在真菌生物膜的形成和毒力中起着关键作用。转录组学和遗传学分析进一步表明,这种活性与细胞内囊泡运输机制有关,特别是ESCRT途径,因为该途径的突变改变了对EntV肽的敏感性并调节了毒力。我们还发现,EntV治疗显著降低了白色念珠菌的EV分泌,支持了一种通过抑制EV介导的毒力来抗真菌的新机制。这些发现进一步表明,EntV是一种有前景的抗毒剂,具有治疗耐药真菌病原体的潜力。
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来源期刊
PLoS Pathogens
PLoS Pathogens MICROBIOLOGY-PARASITOLOGY
自引率
3.00%
发文量
598
期刊介绍: Bacteria, fungi, parasites, prions and viruses cause a plethora of diseases that have important medical, agricultural, and economic consequences. Moreover, the study of microbes continues to provide novel insights into such fundamental processes as the molecular basis of cellular and organismal function.
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