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Drosophila S2 cells: an alternative infection model for Listeria monocytogenes

机译:果蝇S2细胞:李斯特菌李斯特菌的替代感染模型

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Listeria monocytogenes is a Gram-positive facultative intracellular bacterial pathogen that infects humans and animals. Its pathogenic strategy involves the expression of virulence proteins that mediate intracytosolic growth and cell-to-cell spread. A key virulence protein is the cholesterol-dependent cytolysin, listeriolysin O (LLO), which is largely responsible for mediating escape from the phagosome into the host cytosol. To study further the host processes exploited during L. monocytogenes infection, we sought to develop Drosophila S2 cells as a model for infection. Here, we show that S2 cells share a number of properties with mammalian cell culture models of infection. As with mouse macrophages, LLO was required for phagosomal escape from S2 cells. Furthermore, vacuolar escape was dependent on their acidification via the ATPase proton pumps, as bafilomycin A_1 treatment sharply decreased escape. However, unlike in mouse macrophages, LLO mutants replicated in the phagosome of S2 cells. Drosophila cells are cholesterol auxotrophs, and exogenous cholesterol increased the infection rate of L. monocytogenes (LLO independent) and also augmented the efficiency of vacuolar escape (LLO dependent). With available genetic tools such as RNA interference, S2 cells could become an important model in the study of host-pathogen interactions.
机译:单核细胞增生李斯特菌是感染人类和动物的革兰氏阳性兼性细胞内细菌病原体。其致病策略涉及介导胞内生长和细胞间扩散的毒性蛋白的表达。关键毒力蛋白是胆固醇依赖性溶血素,李斯特菌溶血素O(LLO),主要负责介导从吞噬体逃逸到宿主细胞质中。为了进一步研究在单核细胞增生李斯特氏菌感染过程中利用的宿主过程,我们试图开发果蝇S2细胞作为感染模型。在这里,我们显示S2细胞与哺乳动物感染细胞培养模型具有许多特性。与小鼠巨噬细胞一样,吞噬体从S2细胞逃逸也需要LLO。此外,液泡逃逸取决于它们通过ATPase质子泵的酸化作用,因为bafilomycin A_1处理可大大降低逃逸率。但是,与小鼠巨噬细胞不同,LLO突变体在S2细胞的吞噬体中复制。果蝇细胞是胆固醇营养缺陷型,外源胆固醇增加了单核细胞增生李斯特氏菌的感染率(不依赖LLO),也增加了液泡逃逸的效率(依赖LLO)。借助RNA干扰等可用的遗传工具,S2细胞可能成为研究宿主与病原体相互作用的重要模型。

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