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Antibodies protect against intracellular bacteria by FC receptor-mediated lysosomal targeting

机译:抗体通过FC受体介导的溶酶体靶向保护免受细胞内细菌的侵害

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摘要

The protective effect of antibodies (Abs) is generally attributed to neutralization or complement activation. Using Legionella pneu-mophila and Mycobacterium bovis bacillus Calmette-Guerin as a model, we discovered an additional mechanism of Ab-mediated protection effective against intracellular pathogens that normally evade lysosomal fusion. We show that Fc receptor (FcR) engagement by Abs, which can be temporally and spatially separated from bacterial infection, renders the host cell nonpermissive for bacterial replication and targets the pathogens to lysosomes. This process is strictly dependent on kinases involved in FcR signaling but not on host cell protein synthesis or protease activation. Based on these findings, we propose a mechanism whereby Abs and FcR engagement subverts the strategies by which intracellular bacterial pathogens evade lysosomal degradation.
机译:抗体(Abs)的保护作用通常归因于中和或补体激活。使用嗜肺军团菌和牛分枝杆菌卡介特-Guerin作为模型,我们发现了Ab介导的保护机制,可有效防御通常逃避溶酶体融合的细胞内病原体。我们显示Abs的Fc受体(FcR)参与,可以在时间和空间上与细菌感染分离,使宿主细胞不允许细菌复制,并将病原体靶向溶酶体。该过程严格依赖于参与FcR信号传导的激酶,而不依赖于宿主细胞蛋白质合成或蛋白酶活化。基于这些发现,我们提出了一种机制,其中Abs和FcR参与颠覆了细胞内细菌病原体规避溶酶体降解的策略。

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