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新型隐球菌产生的生物膜可保护该真菌免受环孢素的抗真菌和抗黑色素作用的影响。

The biofilm produced by Cryptococcus neoformans protects the fungus from the antifungal and anti-melanin effects of cyclosporine.

作者信息

Andrade Iara Bastos de, Alves Vinícius, Correa-Junior Dario, Avellar-Moura Igor, Soares Juliana, Sousa Araújo Glauber Ribeiro de, Pontes Bruno, Nosanchuk Joshua D, Almeida-Paes Rodrigo, Frases Susana

机构信息

Laboratório de Biofísica de Fungos, Instituto de Biofísica Carlos Chagas Filho, Universidade Federal do Rio de Janeiro, Rio de Janeiro, RJ, Brazil.

Laboratório de Biofísica de Fungos, Instituto de Biofísica Carlos Chagas Filho, Universidade Federal do Rio de Janeiro, Rio de Janeiro, RJ, Brazil; Departments of Medicine (Division of Infectious Diseases) and Microbiology and Immunology, Albert Einstein College of Medicine, Bronx, NY, USA.

出版信息

Microb Pathog. 2025 Jan;198:107124. doi: 10.1016/j.micpath.2024.107124. Epub 2024 Nov 15.

Abstract

Understanding Cryptococcus neoformans pathogenesis requires a detailed analysis of the various virulence factors that contribute to its ability to cause disease. Cyclosporine, calcineurin inhibitor, impairs C. neoformans production of a polysaccharide capsule and secretion of urease, which are critical for cryptococcal pathogenesis. Two particularly important virulence factors are the production of cell wall melanin and formation of biofilm. In this study, we investigated cyclosporine's effects on melanin production and biofilm formation in C. neoformans. Initially, we examined melanin production in planktonic cells treated with cyclosporine using an L-DOPA containing melanin-inducing medium. Visual inspection and optical microscopy revealed a notable reduction in the characteristic dark coloration of cultures treated with cyclosporine, which indicate decreased melanin production in daughter cells compared to mother cells. Spectrophotometric analysis also demonstrated a significantly altered ultraviolet-visible (UV/vis) absorption spectra in cyclosporine-treated yeast cells, indicative of structural changes in melanin. Additionally, cyclosporine-treated cells exhibited reduced conductance (P-value < 0.0001), suggesting altered cellular ionic properties. The impact of cyclosporine on biofilm formation and mature biofilm disruption was also assessed. Despite cyclosporine's efficacy in modifying virulence factors during planktonic growth, cyclosporine did not inhibit biofilm formation or melanization under biofilm growth conditions, nor did it disrupt mature biofilms in terms of biomass or metabolic activity. However, there was a significant reduction in extracellular matrix production in cyclosporine-treated non-melanized biofilms. Our findings underscore the complex interplay between cyclosporine and C. neoformans, highlighting its differential effects on melanization and biofilm dynamics, which provides new insights into the shortcomings of cyclosporin for combatting cryptococcosis and informs pathways for future therapeutic strategies against cryptococcosis.

摘要

了解新型隐球菌的发病机制需要详细分析各种有助于其致病能力的毒力因子。环孢素,一种钙调神经磷酸酶抑制剂,会损害新型隐球菌多糖荚膜的产生和脲酶的分泌,而这些对于隐球菌的发病机制至关重要。两个特别重要的毒力因子是细胞壁黑色素的产生和生物膜的形成。在本研究中,我们调查了环孢素对新型隐球菌黑色素产生和生物膜形成的影响。最初,我们使用含L-多巴的黑色素诱导培养基检查了用环孢素处理的浮游细胞中的黑色素产生情况。目视检查和光学显微镜显示,用环孢素处理的培养物特征性深色显著减少,这表明与母细胞相比,子细胞中的黑色素产生减少。分光光度分析还表明,经环孢素处理的酵母细胞的紫外可见(UV/vis)吸收光谱发生了显著变化,这表明黑色素的结构发生了变化。此外,经环孢素处理的细胞表现出导电性降低(P值<0.0001),表明细胞离子特性发生了改变。还评估了环孢素对生物膜形成和成熟生物膜破坏的影响。尽管环孢素在浮游生长过程中有效改变毒力因子,但在生物膜生长条件下,环孢素既不抑制生物膜形成也不抑制黑色素化,在生物量或代谢活性方面也不破坏成熟生物膜。然而,经环孢素处理的非黑色素化生物膜的细胞外基质产生显著减少。我们的研究结果强调了环孢素与新型隐球菌之间复杂的相互作用,突出了其对黑色素化和生物膜动态的不同影响,这为环孢素治疗隐球菌病的缺点提供了新的见解,并为未来抗隐球菌病治疗策略的途径提供了信息。

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