Mucci D, Forristal J, Strickland D, Morris R, Fitzgerald D, Saelinger C B
Department of Molecular Genetics, University of Cincinnati, College of Medicine, Ohio 45267, USA.
Infect Immun. 1995 Aug;63(8):2912-8. doi: 10.1128/iai.63.8.2912-2918.1995.
Pseudomonas exotoxin A (PE) enters mammalian cells via a receptor-mediated endocytic pathway. The initial step in this pathway is binding to the multiligand receptor termed the alpha 2-macroglobulin receptor/low-density lipoprotein receptor-related protein (LRP). Binding of toxin, and of the many other ligands that bind to LRP, is blocked by the addition of a 39-kDa receptor-associated protein (RAP). Here we show that approximately 40% of the cell-associated LRP is on the surface of toxin-sensitive mouse LM fibroblasts and thus accessible for toxin internalization. The remainder is located intracellularly, primarily in the Golgi region. Mammalian cells exhibit a wide range of sensitivity to PE. To investigate possible reasons for this, we examined the expression levels of both LRP and RAP. Results from a variety of cell lines indicated that there was a positive correlation between LRP expression and toxin sensitivity. In the absence of LRP, cells were as much as 200-fold more resistant to PE compared with sensitive cells. A second group of resistant cells expressed LRP but had a high level of RAP. Thus, a toxin-resistant phenotype would be expected when cells expressed either low levels of LRP or high levels of LRP in the presence of high levels of RAP. We hypothesize that RAP has a pivotal role in moderating cellular susceptibility to PE.
铜绿假单胞菌外毒素A(PE)通过受体介导的内吞途径进入哺乳动物细胞。该途径的第一步是与称为α2-巨球蛋白受体/低密度脂蛋白受体相关蛋白(LRP)的多配体受体结合。毒素以及许多其他与LRP结合的配体的结合会被添加一种39 kDa的受体相关蛋白(RAP)所阻断。在此我们表明,约40%与细胞相关的LRP位于对毒素敏感的小鼠LM成纤维细胞表面,因此可用于毒素内化。其余部分位于细胞内,主要在高尔基体区域。哺乳动物细胞对PE表现出广泛的敏感性。为了探究其可能的原因,我们检测了LRP和RAP的表达水平。来自多种细胞系的结果表明,LRP表达与毒素敏感性之间存在正相关。在缺乏LRP的情况下,与敏感细胞相比,细胞对PE的抗性高达200倍。第二组抗性细胞表达LRP,但RAP水平较高。因此,当细胞表达低水平的LRP或在高水平RAP存在的情况下表达高水平的LRP时,预计会出现毒素抗性表型。我们推测RAP在调节细胞对PE的敏感性方面具有关键作用。
