ATP 依赖性铜绿假单胞菌外毒素从淋巴细胞中毒过程中晚期再循环区室的转运参与情况。
Involvement of ATP-dependent Pseudomonas exotoxin translocation from a late recycling compartment in lymphocyte intoxication procedure.
作者信息
Alami M, Taupiac M P, Reggio H, Bienvenüe A, Beaumelle B
机构信息
UMR 5539 Centre National de la Recherche Scientifique, Département Biologie-Santé, Université Montpellier II, Montpellier, France.
出版信息
Mol Biol Cell. 1998 Feb;9(2):387-402. doi: 10.1091/mbc.9.2.387.
Pseudomonas exotoxin (PE) is a cytotoxin which, after endocytosis, is delivered to the cytosol where it inactivates protein synthesis. Using diaminobenzidine cytochemistry, we found over 94% of internalized PE in transferrin (Tf) -positive endosomes of lymphocytes. When PE translocation was examined in a cell-free assay using purified endocytic vesicles, more than 40% of endosomal 125I-labeled PE was transported after 2 h at 37 degrees C, whereas a toxin inactivated by point mutation in its translocation domain was not translocated. Sorting of endosomes did not allow cell-free PE translocation, whereas active PE transmembrane transport was observed after > 10 min of endocytosis when PE and fluorescent-Tf were localized by confocal immunofluorescence microscopy within a rab5-positive and rab4- and rab7-negative recycling compartment in the pericentriolar region of the cell. Accordingly, when PE delivery to this structure was inhibited using a 20 degrees C endocytosis temperature, subsequent translocation from purified endosomes was impaired. Translocation was also inhibited when endosomes were obtained from cells labeled with PE in the presence of brefeldin A, which caused fusion of translocation-competent recycling endosomes with translocation-incompetent sorting elements. No PE processing was observed in lymphocyte endosomes, the full-sized toxin was translocated and recovered in an enzymatically active form. ATP hydrolysis was found to directly provide the energy required for PE translocation. Inhibitors of endosome acidification (weak bases, protonophores, or bafilomycin A1) when added to the assay did not significantly affect 125I-labeled PE translocation, demonstrating that this transport is independent of the endosome-cytosol pH gradient. Nevertheless, when 125I-labeled PE endocytosis was performed in the presence of one of these molecules, translocation from endosomes was strongly inhibited, indicating that exposure to acidic pH is a prerequisite for PE membrane traversal. When applied during endocytosis, treatments that protect cells against PE intoxication (low temperatures, inhibitors of endosome acidification, and brefeldin A) impaired 125I-labeled PE translocation from purified endosomes. We conclude that PE translocation from a late receptor recycling compartment is implicated in the lymphocyte intoxication procedure.
铜绿假单胞菌外毒素(PE)是一种细胞毒素,经内吞作用后被转运至胞质溶胶,在那里它会使蛋白质合成失活。利用二氨基联苯胺细胞化学技术,我们发现超过94%内化的PE存在于淋巴细胞的转铁蛋白(Tf)阳性内体中。当在使用纯化内吞小泡的无细胞测定中检测PE转位时,在37℃下2小时后,超过40%的内体125I标记的PE被转运,而其转位结构域中因点突变而失活的毒素则未发生转位。内体的分选不允许无细胞的PE转位,而当通过共聚焦免疫荧光显微镜观察到PE和荧光Tf在内吞作用>10分钟后位于细胞中心粒周围区域的rab5阳性且rab4和rab7阴性的再循环区室中时,观察到了活跃的PE跨膜转运。因此,当使用20℃的内吞温度抑制PE向该结构的递送时,随后从纯化内体的转位受损。当在布雷菲德菌素A存在下从用PE标记的细胞中获得内体时,转位也受到抑制,布雷菲德菌素A会导致具有转位能力的再循环内体与无转位能力的分选元件融合。在淋巴细胞内体中未观察到PE的加工过程,全长毒素发生转位并以酶活性形式回收。发现ATP水解直接提供PE转位所需的能量。当添加到测定中时,内体酸化抑制剂(弱碱、质子载体或巴弗洛霉素A1)对125I标记的PE转位没有显著影响,表明这种转运与内体-胞质溶胶pH梯度无关。然而,当在这些分子之一存在的情况下进行125I标记的PE内吞作用时,从内体的转位受到强烈抑制,表明暴露于酸性pH是PE穿越膜的先决条件。在内吞作用期间应用时,保护细胞免受PE中毒的处理(低温、内体酸化抑制剂和布雷菲德菌素A)会损害125I标记的PE从纯化内体的转位。我们得出结论,PE从晚期受体再循环区室的转位与淋巴细胞中毒过程有关。
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