首页> 美国卫生研究院文献>Infection and Immunity >A Candida albicans Mannoprotein Deprived of Its Mannan Moiety Is Efficiently Taken Up and Processed by Human Dendritic Cells and Induces T-Cell Activation without Stimulating Proinflammatory Cytokine Production
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A Candida albicans Mannoprotein Deprived of Its Mannan Moiety Is Efficiently Taken Up and Processed by Human Dendritic Cells and Induces T-Cell Activation without Stimulating Proinflammatory Cytokine Production

机译:缺少甘露聚糖部分的白色念珠菌甘露糖蛋白可被人类树突状细胞有效摄取并加工并诱导T细胞活化而不会刺激促炎性细胞因子的产生。

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摘要

Mannoproteins are cell wall components of pathogenic fungi and play major virulence and immunogenic roles with both their mannan and protein moieties. The 65-kDa mannoprotein (MP65) of Candida albicans is a β-glucanase adhesin recognized as a major target of the human immune response against this fungus, and its recombinant product (rMP65; devoid of the mannan moiety) is presently under consideration as a vaccine candidate. Here we investigated cellular and molecular aspects of the interaction of rMP65 with human antigen-presenting cells. We also assessed the ability of rMP65 to initiate a T-cell response. Both the native mannosylated MP65 (nMP65) and the recombinant product were efficiently bound and taken up by macrophages and dendritic cells. However, contrarily to nMP65, rMP65 did not induce tumor necrosis factor alpha and interleukin-6 release from these cells. On the other hand, rMP65 was rapidly endocytosed by both macrophages and dendritic cells, in a process involving both clathrin-dependent and clathrin-independent mechanisms. Moreover, the RGD sequence inhibited rMP65 uptake to some extent. After internalization, rMP65 partially colocalized with lysosomal membrane-associated glycoproteins 1 and 2. This possibly resulted in efficient protein degradation and presentation to CD4+ T cells, which proliferated and produced gamma interferon. Collectively, these results demonstrate that the absence of the mannan moiety does not deprive MP65 of the capacity to initiate the pattern of cellular and molecular events leading to antigen presentation and T-cell activation, which are essential features for further consideration of MP65 as a potential vaccine candidate.
机译:甘露糖蛋白是致病性真菌的细胞壁成分,其甘露聚糖和蛋白质部分均起主要毒力和免疫原性作用。白色念珠菌的65 kDa甘露糖蛋白(MP65)是一种β-葡聚糖酶黏附素,被认为是人类针对这种真菌的免疫反应的主要靶标,目前正在考虑将其重组产物(rMP65;不含甘露聚糖部分)作为候选疫苗。在这里,我们研究了rMP65与人类抗原呈递细胞相互作用的细胞和分子方面。我们还评估了rMP65启动T细胞反应的能力。天然的甘露糖基化的MP65(nMP65)和重组产物均被巨噬细胞和树突状细胞有效结合并吸收。但是,与nMP65相反,rMP65不会诱导肿瘤坏死因子α和白细胞介素6从这些细胞中释放。另一方面,在涉及网格蛋白依赖性和网格蛋白依赖性机制的过程中,rMP65被巨噬细胞和树突状细胞快速内吞。而且,RGD序列在一定程度上抑制了rMP65的摄取。内化后,rMP65与溶酶体膜相关糖蛋白1和2部分共定位。这可能导致有效的蛋白质降解并呈递给CD4 + T细胞,从而增殖并产生γ干扰素。总的来说,这些结果表明,缺少甘露聚糖部分并不能使MP65丧失引发导致抗原呈递和T细胞活化的细胞和分子事件的模式的能力,这是进一步考虑将MP65视为潜在分子的基本特征。候选疫苗。

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