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Impaired cross-presentation of CD8α +CD11c + dendritic cells by Japanese encephalitis virus in a TLR2/MyD88 signal pathway-dependent manner

机译:受损cross-presentation CD8α+ CD11c +树突细胞由日本脑炎病毒TLR2 / MyD88信号pathway-dependent方式

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摘要

Cross-presentation is the pathway by which exogenous antigens are routed for presentation by MHC class I molecules leading to activation of antiviral CD8 + T-cell responses. However, there is little information describing the modulation of cross-presentation and the impact of pathogen-derived signals associated with Japanese encephalitis virus (JEV), which is one of the most common causes of encephalitis in humans. In this study, we demonstrate that JEV infection could suppress in vivo cross-presentation of soluble and cell-associated antigens, thereby generating weak CD8 + T-cell responses to exogenous antigens, as evaluated by CFSE dilution of adoptively transferred CD8 + T cells and in vivo CTL killing activity. Furthermore, CD8α +CD11c + dendritic cells (DCs), which are known to be far more efficient at cross-presenting soluble antigens, played a specific role in contributing to JEV-mediated inhibition of the cross-presentation of exogenous antigens through interference with effective antigen uptake. Finally, this study provides evidence that TLR2-MyD88 and p38 MAPK signal pathway might be involved in JEV-mediated inhibition of cross-presentation of soluble and cell-associated antigens. These observations suggest that the modulation of cross-presentation of exogenous antigens through TLR signaling has important implications for antiviral immune responses against JEV infection and the development of effective vaccination strategies.
机译:Cross-presentation的途径提示外源性抗原路由我类MHC分子的激活抗病毒CD8 + t细胞反应。没有信息描述调制cross-presentation和所带来的影响pathogen-derived信号与日本有关脑炎病毒(JEV),这是其中的一个脑炎在人类身上的最常见原因。这项研究中,我们证明了JEV感染会抑制体内cross-presentation的溶性和细胞相关抗原,从而生成弱CD8 + t细胞反应外源性抗原,如评估CFSE稀释收养的CD8 + T细胞在转移体内CTL杀人活动。+ CD11c +树突状细胞(dc)是已知的在cross-presenting更有效可溶性抗原,发挥了特殊作用导致JEV-mediated抑制的cross-presentation外源性抗原干扰有效抗原摄取。最后,该研究提供了证据TLR2-MyD88和p38 MAPK信号通路参与JEV-mediated抑制cross-presentation可溶性细胞相关抗原。调制cross-presentation外生的通过TLR信号具有重要的抗原对抗病毒免疫反应的影响针对JEV感染和的发展有效的疫苗接种战略。

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