首页> 美国卫生研究院文献>PLoS Pathogens >Macrophages protect Talaromyces marneffei conidia from myeloperoxidase-dependent neutrophil fungicidal activity during infection establishment in vivo
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Macrophages protect Talaromyces marneffei conidia from myeloperoxidase-dependent neutrophil fungicidal activity during infection establishment in vivo

机译:巨噬细胞在体内感染建立过程中保护马尔尼菲分枝杆菌免受髓过氧化物酶依赖性中性粒细胞杀真菌活性

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摘要

Neutrophils and macrophages provide the first line of cellular defence against pathogens once physical barriers are breached, but can play very different roles for each specific pathogen. This is particularly so for fungal pathogens, which can occupy several niches in the host. We developed an infection model of talaromycosis in zebrafish embryos with the thermally-dimorphic intracellular fungal pathogen Talaromyces marneffei and used it to define different roles of neutrophils and macrophages in infection establishment. This system models opportunistic human infection prevalent in HIV-infected patients, as zebrafish embryos have intact innate immunity but, like HIV-infected talaromycosis patients, lack a functional adaptive immune system. Importantly, this new talaromycosis model permits thermal shifts not possible in mammalian models, which we show does not significantly impact on leukocyte migration, phagocytosis and function in an established Aspergillus fumigatus model. Furthermore, the optical transparency of zebrafish embryos facilitates imaging of leukocyte/pathogen interactions in vivo. Following parenteral inoculation, T. marneffei conidia were phagocytosed by both neutrophils and macrophages. Within these different leukocytes, intracellular fungal form varied, indicating that triggers in the intracellular milieu can override thermal morphological determinants. As in human talaromycosis, conidia were predominantly phagocytosed by macrophages rather than neutrophils. Macrophages provided an intracellular niche that supported yeast morphology. Despite their minor role in T. marneffei conidial phagocytosis, neutrophil numbers increased during infection from a protective CSF3-dependent granulopoietic response. By perturbing the relative abundance of neutrophils and macrophages during conidial inoculation, we demonstrate that the macrophage intracellular niche favours infection establishment by protecting conidia from a myeloperoxidase-dependent neutrophil fungicidal activity. These studies provide a new in vivo model of talaromycosis with several advantages over previous models. Our findings demonstrate that limiting T. marneffei’s opportunity for macrophage parasitism and thereby enhancing this pathogen’s exposure to effective neutrophil fungicidal mechanisms may represent a novel host-directed therapeutic opportunity.
机译:一旦突破了物理障碍,嗜中性粒细胞和巨噬细胞将成为抵抗病原体的第一道防线,但对于每种特定的病原体,它们可以发挥非常不同的作用。对于真菌病原体而言尤其如此,其可以在宿主中占据几个小生境。我们开发了斑马鱼胚胎中的拟南芥胞内热变态性真菌病原菌Talaromyces marneffei的感染模型,并用它来定义嗜中性粒细胞和巨噬细胞在感染建立中的不同作用。该系统模拟了在HIV感染患者中普遍存在的机会性人类感染,因为斑马鱼胚胎具有完整的先天免疫力,但是像HIV感染的滑石病患者一样,缺乏功能适应性免疫系统。重要的是,这种新的talalomycosis模型允许在哺乳动物模型中不可能发生热转移,在已建立的烟曲霉模型中,我们证明这对白细胞迁移,吞噬作用和功能没有显着影响。此外,斑马鱼胚胎的光学透明性有助于体内白细胞/病原体相互作用的成像。肠胃外接种后,嗜中性粒细胞和巨噬细胞均吞噬了马尔尼菲分生孢子。在这些不同的白细胞中,细胞内的真菌形式各不相同,这表明细胞内环境中的触发因素可以覆盖热形态学决定因素。如在人类滑囊菌病中,分生孢子主要被巨噬细胞而不是嗜中性白细胞吞噬。巨噬细胞提供了支持酵母形态的细胞内利基。尽管它们在T. marneffei分生孢子的吞噬作用中起着较小的作用,但在感染过程中,中性粒细胞的数量却因保护性的CSF3依赖性颗粒生成反应而增加。通过在分生孢子接种过程中干扰嗜中性粒细胞和巨噬细胞的相对丰度,我们证明巨噬细胞的细胞内利基通过保护分生孢子免受髓过氧化物酶依赖性嗜中性白细胞的杀真菌活性而有利于感染的建立。这些研究提供了一种新的滑石粉体内模型,与以前的模型相比具有多个优点。我们的发现表明,限制Marneffei噬菌体发生巨噬细胞寄生虫的机会,从而增加这种病原体对有效的中性粒细胞杀真菌剂的暴露程度,可能是一种新颖的宿主定向治疗机会。

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