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Anthrax Toxin Entry into Polarized Epithelial Cells

机译:炭疽毒素进入极化上皮细胞

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We examined the entry of anthrax edema toxin (EdTx) into polarized human T84 epithelial cells using cyclic AMP-regulated Cl?secretion as an index of toxin entry. EdTx is a binary A/B toxin which self assembles at the cell surface from anthrax edema factor and protective antigen (PA). PA binds to cell surface receptors and delivers EF, an adenylate cyclase, to the cytosol. EdTx elicited a strong Cl? secretory response when it was applied to the basolateral surface of T84 cells but no response when it was applied to the apical surface. PA alone had no effect when it was applied to either surface. T84 cells exposed basolaterally bound at least 30-fold-more PA than did T84 cells exposed apically, indicating that the PA receptor is largely or completely restricted to the basolateral membrane of these cells. The PA receptor did not fractionate with detergent-insoluble caveola-like membranes as cholera toxin receptors do. These findings have implications regarding the nature of the PA receptor and confirm the view that EdTx and CT coopt fundamentally different subcellular systems to enter the cell and cause disease.
机译:我们使用环状AMP调节的Cl ?分泌作为毒素进入的指标,检查了炭疽水肿毒素(EdTx)进入极化的人类T84上皮细胞的进入。 EdTx是一种二元A / B毒素,可通过炭疽浮肿因子和保护性抗原(PA)在细胞表面自组装。 PA与细胞表面受体结合并将EF(腺苷酸环化酶)传递到细胞质中。 EdTx应用于T84细胞的基底外侧表面时,会引起强烈的Cl ?分泌反应,而应用于顶部表面时则没有反应。仅将PA应用于任一表面都没有效果。与顶部暴露的T84细胞相比,基底外侧暴露的T84细胞结合的PA至少多30倍,这表明PA受体在很大程度上或完全局限于这些细胞的基底外侧膜。与霍乱毒素受体不同,PA受体不能与去污剂不溶的海绵状膜分离。这些发现暗示了PA受体的性质,并证实了EdTx和CT共同采用根本不同的亚细胞系统进入细胞并引起疾病的观点。

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