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Subunit S1 of pertussis toxin: mapping of the regions essential for ADP-ribosyltransferase activity.

机译:百日咳毒素的亚基S1:定位ADP-核糖基转移酶活性必不可少的区域。

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摘要

The toxicity of pertussis toxin is mediated by the ADP-ribosyltransferase activity of subunit S1. To understand the structure-function relationship of subunit S1 and guide the construction of nontoxic molecules suitable for vaccines, we constructed and expressed in Escherichia coli a series of amino-terminal and carboxyl-terminal deletion mutants as well as a number of molecules containing amino acid substitutions. The shortest peptide still retaining enzymatic activity contains amino acids 2-179. Within this region we identified three mutants in which amino acid substitutions abolish the enzymatic activity. Mutation of amino acids 8 and 9 or 50 and 53, located within the region of the S1 subunit of pertussis toxin homologous to cholera toxin, causes loss of enzymatic activity. Outside this homology region, substitution of Glu-129 with glycine or aspartic acid also eliminates the enzymatic activity of the S1 subunit. In this respect, Glu-129 resembles the glutamic acid that is crucial for the catalytic activity of diphtheria and Pseudomonas toxins. Once introduced into the Bordetella pertussis chromosome, the above mutations should lead to the synthesis of nontoxic pertussis toxin molecules suitable for vaccine production.
机译:百日咳毒素的毒性是由亚基S1的ADP-核糖基转移酶活性介导的。为了了解亚基S1的结构-功能关系并指导适用于疫苗的无毒分子的构建,我们在大肠杆菌中构建并表达了一系列氨基末端和羧基末端缺失突变体以及许多含有氨基酸的分子换人。仍保留酶促活性的最短肽包含氨基酸2-179。在该区域内,我们鉴定了三个突变体,其中氨基酸取代消除了酶促活性。位于与霍乱毒素同源的百日咳毒素的S1亚基区域内的氨基酸8和9或50和53的突变引起酶活性的损失。在该同源性区域之外,用甘氨酸或天冬氨酸取代Glu-129也消除了S1亚基的酶促活性。在这方面,Glu-129类似于谷氨酸,对白喉和假单胞菌毒素的催化活性至关重要。一旦引入百日咳博德特氏菌染色体,上述突变应导致合成适合疫苗生产的无毒百日咳毒素分子。

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