内体酶和溶酶体酶降解蓖麻毒素A链——蓖麻毒素B链的保护作用。

Therapeutic immunology Pub Date : 1994-08-01
A Bilge, J Howell-Clark, S Ramakrishnan, O W Press
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引用次数: 0

摘要

我们研究了蛋白水解酶在细胞内加工蓖麻毒素A链(RTA)对其核糖体抑制活性表达的作用。从Jurkat细胞中提取的内体和溶酶体蛋白酶以及纯化的组织蛋白酶B、D和G与RTA孵育,通过蛋白水解裂解产生28 kda的片段。这一过程与胞内蛋白酶裂解假单胞菌外毒素和白喉毒素产生具有功能活性的毒素片段相似。然而,纯化的RTA 28kda片段的核糖体抑制活性比天然RTA低11000倍,这表明这种切割不是毒素细胞毒性活性的必要步骤。在降解实验中加入蓖麻毒素B链(ricin B chain, RTB)可使其免受溶酶体和组织蛋白酶的蛋白水解作用。然而,RTB没有保护另一种RNA作用蛋白RNAase;过量的未标记的RTA或IgG也不能保护标记的RTA免受降解,这表明RTB的保护作用是其与RTA相互作用所特有的。这种对RTB的保护作用可能部分解释了含有整个蓖麻毒素的免疫毒素(ITs)比只含有RTA的免疫毒素毒性更高的原因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Degradation of ricin A chain by endosomal and lysosomal enzymes--the protective role of ricin B chain.

We investigated the role of intracellular processing of ricin A chain (RTA) by proteolytic enzymes on the expression of its ribosome inhibitory activity. Endosomal and lysosomal proteases extracted from Jurkat cells and purified cathepsins B, D and G were incubated with RTA, resulting in generation of a 28-kDa fragment by proteolytic cleavage. This process was reminiscent of the nicking of Pseudomonas exotoxin and Diphtheria toxin by intracellular proteases to produce functionally active toxin fragments. However, the ribosome inhibitory activity of the purified 28-kDa fragment of RTA was 11,000-fold less than that of native RTA, suggesting that such cleavage is not an essential step in the cytotoxic activity of the toxin. Addition of ricin B chain (RTB) in degradation assays resulted in the protection of RTA from proteolytic activities of lysosomes and cathepsins. However, RTB did not protect another RNA acting protein, RNAase; nor did excess amounts of unlabeled RTA or IgG protect labelled RTA from degradation, suggesting that the protective effect of RTB was specific to its interaction with RTA. Such a protective role for RTB may partially account for the higher toxicity of immunotoxins (ITs) containing whole ricin compared to ITs containing only RTA.

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