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低pH环境在腺病毒增强铜绿假单胞菌外毒素-表皮生长因子偶联物毒性中的作用

Role of a low-pH environment in adenovirus enhancement of the toxicity of a Pseudomonas exotoxin-epidermal growth factor conjugate.

作者信息

Seth P, Fitzgerald D J, Willingham M C, Pastan I

出版信息

J Virol. 1984 Sep;51(3):650-5. doi: 10.1128/JVI.51.3.650-655.1984.

Abstract

A conjugate of Pseudomonas exotoxin and epidermal growth factor (PE-EGF) inhibits proteins synthesis in KB cells, and this inhibition is increased by adenovirus. Protein synthesis inhibition is dependent on the amount of adenovirus and PE-EGF used and the time of incubation of cells with these agents. With 1 microgram of adenovirus and 0.5 micrograms of PE-EGF per ml, protein synthesis is inhibited about 80% in a 60-min experiment. Under these conditions neither adenovirus nor PE-EGF alone has any effect. In the presence of several weak bases or monensin, the enhancement of toxicity was substantially inhibited; half-maximal inhibition was achieved with 40 microM chloroquine, 10 mM ammonium chloride, 5 mM methylamine, 0.1 mM N-hexylamine and 1 microM monensin. At the concentrations employed, none of the inhibitors affected the amount of virus taken up or bound to the cell surface, and chloroquine had no effect on the amount of EGF taken up in 60 min. Chloroquine did not prevent the toxicity of the PE-EGF (5 micrograms/ml) alone. Because these compounds are known to elevate the pH in receptosomes, it seems likely that the acidification of the receptosome either enhances the lysis of the membrane by adenovirus or enhances some other step in the release of PE-EGF.

摘要

铜绿假单胞菌外毒素与表皮生长因子的偶联物(PE - EGF)可抑制KB细胞中的蛋白质合成,而腺病毒可增强这种抑制作用。蛋白质合成抑制作用取决于所用腺病毒和PE - EGF的量以及细胞与这些试剂孵育的时间。在每毫升含1微克腺病毒和0.5微克PE - EGF的情况下,在60分钟的实验中蛋白质合成被抑制约80%。在这些条件下,单独的腺病毒或PE - EGF均无任何作用。在存在几种弱碱或莫能菌素的情况下,毒性增强被显著抑制;40微摩尔氯喹、10毫摩尔氯化铵、5毫摩尔甲胺、0.1毫摩尔正己胺和1微摩尔莫能菌素可实现半数最大抑制。在所使用的浓度下,没有一种抑制剂影响细胞摄取或结合到细胞表面的病毒量,并且氯喹对60分钟内摄取的表皮生长因子量没有影响。氯喹不能阻止单独的PE - EGF(5微克/毫升)的毒性。因为已知这些化合物可提高受体小体中的pH值,所以受体小体的酸化似乎要么增强了腺病毒对膜的裂解作用,要么增强了PE - EGF释放中的其他某个步骤。

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