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念珠菌溶素的进化洞察及近期进展。

Insights into the evolution of Candidalysin and recent developments.

作者信息

Konwar Ananya, Mathur Kartavya, Pandey Shivam, Bhorali Kunjan, Thakur Anil, Puria Rekha

机构信息

School of Biotechnology, Gautam Buddha University, Greater Noida, Uttar Pradesh, India.

Regional Centre for Biotechnology, 3rd Milestone Gurgaon- Faridabad Expressway, Faridabad, Haryana, India.

出版信息

Arch Microbiol. 2025 Jul 31;207(9):206. doi: 10.1007/s00203-025-04414-z.

Abstract

The alarming rise in fungal infections poses a serious health concern worldwide. Candida albicans is a highly virulent, ubiquitous opportunistic fungal pathogen associated with high mortality, particularly in immunocompromised individuals. Its infections range from superficial mucosal to invasive candidiasis. The pathogenicity of C. albicans is largely attributed to its ability to undergo phenotypic switching between different morphological forms ranging from unicellular to hyphae. A key factor in its pathogenesis is candidalysin, a fungal cytolytic peptide toxin. Candidalysin is generated through the expression of the ECE1 polyprotein, which, upon cleavage by the protease Kex2, yields both candidalysin and non-candidalysin ECE1-derived peptides. Notably, despite its critical role in virulence, the ECE1 gene is not widely conserved among fungal pathogens and is predominantly restricted to a few Candida species. This review highlights recent advances in understanding candidalysin-mediated cell damage and immune activation pathways, and also provides insights into the evolution of the ECE1 gene and its potential role in the coevolution of C. albicans with its human host.

摘要

真菌感染的惊人增长在全球范围内引发了严重的健康问题。白色念珠菌是一种毒性很强、无处不在的机会性真菌病原体,与高死亡率相关,尤其是在免疫功能低下的个体中。其感染范围从浅表黏膜感染到侵袭性念珠菌病。白色念珠菌的致病性很大程度上归因于其在从单细胞到菌丝的不同形态之间进行表型转换的能力。其发病机制中的一个关键因素是念珠菌溶素,一种真菌细胞溶解肽毒素。念珠菌溶素是通过ECE1多蛋白的表达产生的,该多蛋白在被蛋白酶Kex2切割后,产生念珠菌溶素和非念珠菌溶素ECE1衍生肽。值得注意的是,尽管ECE1基因在毒力中起关键作用,但它在真菌病原体中并不广泛保守,主要局限于少数念珠菌属物种。这篇综述强调了在理解念珠菌溶素介导的细胞损伤和免疫激活途径方面的最新进展,还提供了对ECE1基因进化及其在白色念珠菌与其人类宿主协同进化中的潜在作用的见解。

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