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NADPH oxidase controls phagosomal pH and antigen cross-presentation in human dendritic cells

机译:NADPH氧化酶控制人类树突状细胞的吞噬体pH和抗原交叉呈递

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摘要

The phagocyte NADPH oxidase (NOX2) is critical for the bactericidal activity of phagocytic cells and plays a major role in innate immunity. We showed recently that NOX2 activity in mouse dendritic cells (DCs) prevents acidification of phagosomes, promoting antigen cross-presentation. Inorder to investigate the role of NOX2 in the regulation of the phagosomal pH in human DCs, we analyzed the production of reactive oxygen species (ROS) and the phagosomal/endosomal pH in monocyte-derived DCs and macrophages (MØs) from healthy donors or patients with chronic granulomatous disease (CGD). As expected, we found that human MØs acidify their phagosomes more efficiently than human DCs. Accordingly, the expression of the vacuolar proton ATPase (V-H+-ATPase) was higher in MØs than in DCs. Phagosomal ROS production, however, was also higher in MØs than in DCs, due to higher levels of gp91phox expression and recruitment to phagosomes. In contrast, in the absence of active NOX2, the phagosomal and endosomal pH decreased. Both in the presence of a NOX2 inhibitor and in DCs derived from patients with CGD, the cross-presentation of 2 model tumor antigens was impaired. We conclude that NOX2 activity participates in the regulation of the phagosomal and endosomal pH in human DCs, and is required for efficient antigen cross-presentation.
机译:吞噬细胞NADPH氧化酶(NOX2)对于吞噬细胞的杀菌活性至关重要,并且在先天免疫中起主要作用。我们最近显示,小鼠树突状细胞(DC)中的NOX2活性可防止吞噬体酸化,从而促进抗原交叉呈递。为了研究NOX2在调节人类DC吞噬体pH中的作用,我们分析了来自健康供体或患者的单核细胞DC和巨噬细胞(MØs)中活性氧(ROS)的产生以及吞噬体/内体pH的产生患有慢性肉芽肿病(CGD)。正如预期的那样,我们发现人类MØs比人类DC更有效地酸化吞噬体。因此,MØs中液泡质子ATPase(V-H + -ATPase)的表达高于DC。但是,由于gp91phox表达水平较高和募集到吞噬体,MØs的噬菌体ROS产生也高于DC。相反,在没有活性NOX2的情况下,吞噬体和内体pH降低。在存在NOX2抑制剂的情况下以及在具有CGD患者的DC中,两种模型肿瘤抗原的交叉呈递均受到损害。我们得出的结论是,NOX2活性参与人类DC中吞噬体和内体pH的调节,并且是有效抗原交叉呈递所必需的。

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