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Characterization of an antigenic determinant of the glycoprotein that correlates with pathogenicity of rabies virus.

机译:与狂犬病病毒致病性相关的糖蛋白抗原决定簇的表征。

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摘要

The pathogenicity of fixed rabies virus strains for adult mice depends on the presence of an antigenic determinant on the viral glycoprotein. Two virus-neutralizing monoclonal antibodies have been used to identify this determinant. All pathogenic strains of fixed rabies virus bind to these antibodies and are neutralized by them, whereas nonpathogenic strains fail to react with these monoclonal antibodies and are not neutralized by them. Antigenic variants of the rabies virus with altered glycoprotein were selected by growing virus in the presence of one monoclonal antibody, 194-2. All variants that lost their ability to react with this antibody and an additional antibody, 248-8, were found to be nonpathogenic for adult mice. Analysis of tryptic peptides of the glycoproteins of pathogenic parent virus and nonpathogenic variants and the amino acid sequence of a specific variant tryptic peptide revealed that the change in pathogenicity corresponded to an amino acid substitution at position 333 of the glycoprotein molecule. The nucleotide sequence of the nonpathogenic variant glycoprotein gene contained a base change that confirmed the single amino acid substitution in the tryptic peptide replacing arginine-333 in the parental glycoprotein. We conclude that arginine-333 is essential for the integrity of an antigenic determinant and for the ability of rabies viruses to produce lethal infection in adult mice.
机译:狂犬病病毒固定株对成年小鼠的致病性取决于病毒糖蛋白上抗原决定簇的存在。已经使用两种中和病毒的单克隆抗体来鉴定该决定簇。固定狂犬病病毒的所有致病性菌株均与这些抗体结合并被其中和,而非致病性菌株则无法与这些单克隆抗体反应且未被其中和。通过在一种单克隆抗体194-2存在下生长病毒来选择具有改变的糖蛋白的狂犬病毒的抗原变异体。发现所有丧失与该抗体和另一抗体248-8反应能力的变体对成年小鼠均无致病性。分析致病性亲本病毒和非致病性变体的糖蛋白的胰蛋白酶消化肽以及特定变体胰蛋白酶消化肽的氨基酸序列,发现致病性变化对应于糖蛋白分子333位的氨基酸取代。非致病性变异糖蛋白基因的核苷酸序列包含一个碱基变化,证实了胰蛋白酶肽中的单个氨基酸取代取代了亲本糖蛋白中的精氨酸-333。我们得出结论,精氨酸333对于抗原决定簇的完整性以及狂犬病毒在成年小鼠中产生致命感染的能力至关重要。

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