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Oral Mycobiome Analysis of HIV-Infected Patients: Identification of Pichia as an Antagonist of Opportunistic Fungi

机译:HIV感染患者的口服真菌学分析:毕赤酵母作为机会性真菌的拮抗剂的鉴定

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摘要

Oral microbiota contribute to health and disease, and their disruption may influence the course of oral diseases. Here, we used pyrosequencing to characterize the oral bacteriome and mycobiome of 12 HIV-infected patients and matched 12 uninfected controls. The number of bacterial and fungal genera in individuals ranged between 8–14 and 1–9, among uninfected and HIV-infected participants, respectively. The core oral bacteriome (COB) comprised 14 genera, of which 13 were common between the two groups. In contrast, the core oral mycobiome (COM) differed between HIV-infected and uninfected individuals, with Candida being the predominant fungus in both groups. Among Candida species, C. albicans was the most common (58% in uninfected and 83% in HIV-infected participants). Furthermore, 15 and 12 bacteria-fungi pairs were correlated significantly within uninfected and HIV-infected groups, respectively. Increase in Candida colonization was associated with a concomitant decrease in the abundance of Pichia, suggesting antagonism. We found that Pichia spent medium (PSM) inhibited growth of Candida, Aspergillus and Fusarium. Moreover, Pichia cells and PSM inhibited Candida biofilms (P = .002 and .02, respectively, compared to untreated controls). The mechanism by which Pichia inhibited Candida involved nutrient limitation, and modulation of growth and virulence factors. Finally, in an experimental murine model of oral candidiasis, we demonstrated that mice treated with PSM exhibited significantly lower infection score (P = .011) and fungal burden (P = .04) compared to untreated mice. Moreover, tongues of PSM-treated mice had few hyphae and intact epithelium, while vehicle- and nystatin-treated mice exhibited extensive fungal invasion of tissue with epithelial disruption. These results showed that PSM was efficacious against oral candidiasis in vitro and in vivo. The inhibitory activity of PSM was associated with secretory protein/s. Our findings provide the first evidence of interaction among members of the oral mycobiota, and identifies a potential novel antifungal.
机译:口腔微生物群有助于健康和疾病,其破坏可能影响口腔疾病的进程。在这里,我们使用焦磷酸测序来表征12例HIV感染患者的口腔细菌群和霉菌组,并与12例未感染的对照配对。在未感染和感染艾滋病毒的参与者中,个体细菌和真菌属的数量分别在8-14和1-9之间。核心口腔细菌组(COB)包含14个属,其中两组之间共有13个属。相比之下,HIV感染者和未感染者之间的核心口服真菌组(COM)有所不同,念珠菌是两组中的主要真菌。在念珠菌中,白色念珠菌是最常见的(未感染的占58%,艾滋病毒感染的参与者占83%)。此外,未感染组和HIV感染组中分别有15和12对细菌-真菌显着相关。念珠菌定植的增加与毕赤酵母丰度的下降同时出现,表明有拮抗作用。我们发现毕赤酵母废培养基(PSM)抑制念珠菌,曲霉和镰刀菌的生长。而且,毕赤酵母细胞和PSM抑制了念珠菌生物膜(与未处理的对照相比,分别为P = 0.002和0.02)。毕赤酵母抑制念珠菌的机制涉及营养限制,生长和毒力因子的调节。最后,在口腔念珠菌病的小鼠实验模型中,我们证明了与未治疗的小鼠相比,用PSM治疗的小鼠表现出明显更低的感染评分(P = .011)和真菌负荷(P = .04)。此外,经PSM处理的小鼠的舌头几乎没有菌丝和完整的上皮,而经媒介物和制霉菌素处理的小鼠表现出广泛的真菌侵袭组织,并有上皮破坏。这些结果表明PSM对口腔念珠菌病体外体内有效。 PSM的抑制活性与分泌蛋白有关。我们的发现提供了口腔真菌菌群成员之间相互作用的第一个证据,并确定了潜在的新型抗真菌药。

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