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首页> 外文期刊>Eukaryotic cell >The Pathogenic Fungus Paracoccidioides brasiliensis Exports Extracellular Vesicles Containing Highly Immunogenic α-Galactosyl Epitopes
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The Pathogenic Fungus Paracoccidioides brasiliensis Exports Extracellular Vesicles Containing Highly Immunogenic α-Galactosyl Epitopes

机译:巴西病原性真菌Paracoccidioides出口含有高度免疫原性α-半乳糖基抗原决定簇的细胞外囊泡。

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Exosome-like vesicles containing virulence factors, enzymes, and antigens have recently been characterized in fungal pathogens, such as Cryptococcus neoformans and Histoplasma capsulatum. Here, we describe extracellular vesicles carrying highly immunogenic α-linked galactopyranosyl (α-Gal) epitopes in Paracoccidioides brasiliensis. P. brasiliensis is a dimorphic fungus that causes human paracoccidioidomycosis (PCM). For vesicle preparations, cell-free supernatant fluids from yeast cells cultivated in Ham's defined medium-glucose were concentrated in an Amicon ultrafiltration system and ultracentrifuged at 100,000 × g. P. brasiliensis antigens were present in preparations from phylogenetically distinct isolates Pb18 and Pb3, as observed in immunoblots revealed with sera from PCM patients. In an enzyme-linked immunosorbent assay (ELISA), vesicle components containing α-Gal epitopes reacted strongly with anti-α-Gal antibodies isolated from both Chagas' disease and PCM patients, with Marasmius oreades agglutinin (MOA) (a lectin that recognizes terminal α-Gal), but only faintly with natural anti-α-Gal. Reactivity was inhibited after treatment with α-galactosidase. Vesicle preparations analyzed by electron microscopy showed vesicular structures of 20 to 200 nm that were labeled both on the surface and in the lumen with MOA. In P. brasiliensis cells, components carrying α-Gal epitopes were found distributed on the cell wall, following a punctuated confocal pattern, and inside large intracellular vacuoles. Lipid-free vesicle fractions reacted with anti-α-Gal in ELISA only when not digested with α-galactosidase, while reactivity with glycoproteins was reduced after β-elimination, which is indicative of partial O-linked chain localization. Our findings open new areas to explore in terms of host-parasite relationships in PCM and the role played in vivo by vesicle components and α-galactosyl epitopes.
机译:含有致病因子,酶和抗原的外泌体样囊泡最近已在真菌病原体如新隐球菌和荚膜组织胞浆菌中得到鉴定。在这里,我们描述了携带高度免疫原性的α联吡喃半乳糖(α-Gal)表位在巴西副球菌中的细胞外囊泡。巴西假单胞菌是一种双态真菌,可导致人副球菌病(PCM)。对于囊泡制剂,将来自在Ham限定的中等葡萄糖中培养的酵母细胞的无细胞上清液在Amicon超滤系统中浓缩,并以100,000×em进行超速离心。在从系统发育上分离的分离株Pb18和Pb3的制剂中,存在巴西假单胞菌抗原,这是在PCM患者血清中发现的免疫印迹中观察到的。在酶联免疫吸附试验(ELISA)中,含有α-Gal表位的囊泡成分与从恰加斯病和PCM患者分离的抗α-Gal抗体强烈反应,带有马拉斯缪斯的凝集素(MOA)(一种识别末端的凝集素) α-Gal),但只能与天然的抗α-Gal结合使用。用α-半乳糖苷酶处理后反应性受到抑制。通过电子显微镜分析的囊泡制品显示出20-200nm的囊泡结构,其在表面和内腔中都被MOA标记。在巴西假单胞菌细胞中,发现带有α-Gal表位的成分以共聚焦的方式分布在细胞壁上,并位于大的细胞内液泡中。仅在未用α-半乳糖苷酶消化的情况下,无脂质囊泡级分才与ELISA中的抗α-Gal反应,而在β-消除后与糖蛋白的反应性降低,这表明存在部分O-连锁的链定位。我们的发现为探索PCM中宿主与寄生虫的关系以及囊泡成分和α-半乳糖基表位在体内所起的作用开辟了新的领域。

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