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Inhibition of Respiration of Candida albicans by Small Molecules Increases Phagocytosis Efficacy by Macrophages

机译:通过小分子抑制念珠菌醛糖苷的呼吸增加了巨噬细胞的吞噬效果

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Candida albicans adapts to various conditions in different body niches by regulating gene expression, protein synthesis, and metabolic pathways. These adaptive reactions not only allow survival but also influence the interaction with host cells, which is governed by the composition and structure of the fungal cell wall. Numerous studies had shown linkages between mitochondrial functionality, cell wall integrity and structure, and pathogenicity. Thus, we decided to inhibit single complexes of the respiratory chain of C. albicans and to analyze the resultant interaction with macrophages via their phagocytic activity. Remarkably, inhibition of the fungal bc 1 complex by antimycin A increased phagocytosis, which correlated with an increased accessibility of β-glucans. To contribute to mechanistic insights, we performed metabolic studies, which highlighted significant changes in the abundance of constituents of the plasma membrane. Collectively, our results reinforce the strong linkage between fungal energy metabolism and other components of fungal physiology, which also determine the vulnerability to immune defense reactions. IMPORTANCE The yeast Candida albicans is one of the major fungal human pathogens, for which new therapeutic approaches are required. We aimed at enhancements of the phagocytosis efficacy of macrophages by targeting the cell wall structure of C. albicans , as the coverage of the β-glucan layer by mannans is one of the immune escape mechanisms of the fungus. We unambiguously show that inhibition of the fungal bc 1 complex correlates with increased accessibilities of β-glucans and improved phagocytosis efficiency. Metabolic studies proved not only the known direct effects on reactive oxygen species (ROS) production and fermentative pathways but also the clear downregulation of the ergosterol pathway and upregulation of unsaturated fatty acids. The changed composition of the plasma membrane could also influence the interaction with the overlying cell wall. Thus, our work highlights the far-reaching relevance of energy metabolism, indirectly also for host-pathogen interactions, without affecting viability.
机译:Candida albicans通过调节基因表达,蛋白质合成和代谢途径来适应不同体力的各种条件。这些适应性反应不仅允许存活,而且影响与宿主细胞的相互作用,其受真菌细胞壁的组成和结构来控制。许多研究表明了线粒体功能,细胞壁完整性和结构和致病性之间的联系。因此,我们决定通过其吞噬活性分析与巨噬细胞的呼吸链的单一复合物。值得注意的是,通过抗霉素抑制真菌BC 1复合物增加的吞噬作用增加,其与β-葡聚糖的可达性增加相关。为了促进机械洞察力,我们进行了代谢研究,这突出了质膜的丰富成分的显着变化。统称,我们的结果强化了真菌能量代谢和真菌生理其他组分之间的强烈联系,这也决定了免疫防御反应的脆弱性。重要性酵母念珠菌白醛本身是主要的真菌人类病原体之一,需要新的治疗方法。我们旨在通过靶向C. albicans的细胞壁结构来增强巨噬细胞的吞噬功能效果,因为甘露甘露甘露糖族层的覆盖率是真菌的免疫逃逸机制之一。我们明确表明抑制真菌BC1复合物与β-葡聚糖的可见性和改善的吞噬作用效率相关。代谢研究不仅证明了对反应性氧物质(ROS)生产和发酵途径的已知直接影响,而且还证明了Ergosterol途径的透明下调和不饱和脂肪酸的上调。血浆膜的改变组成也可以影响与上覆细胞壁的相互作用。因此,我们的作品突出了能量代谢的深远相关性,也适用于宿主病原体相互作用,而不会影响活力。

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