Cryptococcus neoformans releases proteins during intracellular residence that affect the outcome of the fungal-macrophage interaction.

microLife Pub Date : 2022-01-01 DOI:10.1093/femsml/uqac015
Eric H Jung, Yoon-Dong Park, Quigly Dragotakes, Lia S Ramirez, Daniel Q Smith, Flavia C G Reis, Amanda Dziedzic, Marcio L Rodrigues, Rosanna P Baker, Peter R Williamson, Anne Jedlicka, Arturo Casadevall, Carolina Coelho
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引用次数: 5

Abstract

Cryptococcus neoformans is a facultative intracellular pathogen that can replicate and disseminate in mammalian macrophages. In this study, we analyzed fungal proteins identified in murine macrophage-like cells after infection with C. neoformans. To accomplish this, we developed a protocol to identify proteins released from cryptococcal cells inside macrophage-like cells; we identified 127 proteins of fungal origin in infected macrophage-like cells. Among the proteins identified was urease, a known virulence factor, and others such as transaldolase and phospholipase D, which have catalytic activities that could contribute to virulence. This method provides a straightforward methodology to study host-pathogen interactions. We chose to study further Yeast Oligomycin Resistance (Yor1), a relatively uncharacterized protein belonging to the large family of ATP binding cassette transporter (ABC transporters). These transporters belong to a large and ancient protein family found in all extant phyla. While ABC transporters have an enormous diversity of functions across varied species, in pathogenic fungi they are better studied as drug efflux pumps. Analysis of C. neoformans yor1Δ strains revealed defects in nonlytic exocytosis, capsule size, and dimensions of extracellular vesicles, when compared to wild-type strains. We detected no difference in growth rates and cell body size. Our results indicate that C. neoformans releases a large suite of proteins during macrophage infection, some of which can modulate fungal virulence and are likely to affect the fungal-macrophage interaction.

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新型隐球菌在细胞内停留期间释放蛋白质,影响真菌-巨噬细胞相互作用的结果。
新型隐球菌是一种兼性细胞内病原体,可以在哺乳动物巨噬细胞中复制和传播。在这项研究中,我们分析了感染新生C.后小鼠巨噬细胞样细胞中鉴定的真菌蛋白。为了实现这一目标,我们开发了一种方案来鉴定巨噬细胞样细胞内隐球菌细胞释放的蛋白质;我们在感染的巨噬细胞样细胞中鉴定出127种真菌来源的蛋白。在鉴定的蛋白质中有脲酶,一种已知的毒力因子,以及其他如转醛缩酶和磷脂酶D,它们具有催化活性,可能有助于毒力。这种方法为研究宿主-病原体相互作用提供了一种简单的方法。我们选择进一步研究酵母寡霉素抗性(Yor1),这是一种相对未知的蛋白质,属于ATP结合盒转运蛋白(ABC转运蛋白)大家族。这些转运蛋白属于一个大而古老的蛋白质家族,在所有现存的门中都有发现。虽然ABC转运蛋白在不同物种中具有巨大的功能多样性,但在病原真菌中,它们作为药物外排泵得到了更好的研究。对新生C. yor1Δ菌株的分析显示,与野生型菌株相比,它们在非溶解性胞吐、胶囊大小和细胞外囊泡尺寸方面存在缺陷。我们没有发现生长速度和细胞体大小的差异。我们的研究结果表明,新生C.在巨噬细胞感染过程中释放大量蛋白质,其中一些蛋白质可以调节真菌的毒力,并可能影响真菌与巨噬细胞的相互作用。
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