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Growth of Candida albicans Cells on the Physiologically Relevant Carbon Source Lactate Affects Their Recognition and Phagocytosis by Immune Cells

机译:生理相关碳源乳酸菌上白色念珠菌细胞的生长影响其对免疫细胞的识别和吞噬作用。

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摘要

Candida albicans is a normal resident of the human gastrointestinal and urogenital tracts and also a prevalent fungal pathogen. During both commensalism and infection, it must match the immunological defenses of its host while adapting to environmental cues and the local nutrient status. C. albicans regularly colonizes glucose-poor niches, thereby depending upon alternative carbon sources for growth. However, most studies of host immune responses to C. albicans have been performed on fungal cells grown on glucose, and the extent to which alternative physiologically relevant carbon sources impact innate immune responses has not been studied. The fungal cell wall is decorated with multifarious pathogen-associated molecular patterns and is the main target for recognition by host innate immune cells. Cell wall architecture is both robust and dynamic, and it is dramatically influenced by growth conditions. We found that growth of C. albicans cells on lactate, a nonfermentative carbon source available in numerous anatomical niches, modulates their interactions with immune cells and the resultant cytokine profile. Notably, lactate-grown C. albicans stimulated interleukin-10 (IL-10) production while decreasing IL-17 levels, rendering these cells less visible to the immune system than were glucose-grown cells. This trend was observed in clinical C. albicans isolates from different host niches and from different epidemiological clades. In addition, lactate-grown C. albicans cells were taken up by macrophages less efficiently, but they were more efficient at killing and escaping these phagocytic cells. Our data indicate that carbon source has a major impact upon the C. albicans interaction with the innate immune system.
机译:白色念珠菌是人类胃肠道和泌尿生殖道的正常居民,也是常见的真菌病原体。在共鸣和感染期间,它必须与宿主的免疫防御相匹配,同时适应环境提示和当地营养状况。白色念珠菌有规律地定居在缺乏葡萄糖的壁ni上,从而取决于生长的替代碳源。但是,大多数宿主对白色念珠菌免疫反应的研究都是在葡萄糖生长的真菌细胞上进行的,尚未研究替代性生理相关碳源对先天免疫反应的影响程度。真菌细胞壁装饰有多种病原体相关的分子模式,是宿主先天免疫细胞识别的主要目标。细胞壁结构既坚固又动态,并且受生长条件的影响很大。我们发现,白色念珠菌细胞在乳酸(一种可在许多解剖位点中获得的非发酵碳源)上的生长,调节了它们与免疫细胞的相互作用以及由此产生的细胞因子谱。值得注意的是,乳酸生长的白色念珠菌刺激了白介素10(IL-10)的产生,同时降低了IL-17的水平,与葡萄糖生长的细胞相比,这些细胞对免疫系统的可见性更低。在来自不同宿主壁and和不同流行病学分支的临床白色念珠菌分离物中观察到这种趋势。另外,乳酸生长的白色念珠菌细胞被巨噬细胞吸收的效率较低,但是它们在杀死和逃避吞噬细胞方面更有效。我们的数据表明碳源对白色念珠菌与先天免疫系统的相互作用具有重大影响。

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