两个氨基酸残基赋予人乳头瘤病毒11型一个中和性、构象依赖性表位以型特异性。
Two amino acid residues confer type specificity to a neutralizing, conformationally dependent epitope on human papillomavirus type 11.
作者信息
Ludmerer S W, Benincasa D, Mark G E
机构信息
Merck Research Laboratories, Rahway, New Jersey, USA.
出版信息
J Virol. 1996 Jul;70(7):4791-4. doi: 10.1128/JVI.70.7.4791-4794.1996.
Abstract
Characterization of virus binding by neutralizing antibodies is important both in understanding early events in viral infectivity and in development of vaccines. Neutralizing monoclonal antibodies (MAbs) to human papillomavirus type 11 (HPV11) have been described, but mapping the binding site has been difficult because of the conformational nature of key type-specific neutralization epitopes on the L1 coat protein. We have determined those residues of the L1 protein of HPV11 which confer type specificity to the binding of HPV11-neutralizing MAbs. Binding of three HPV11-specific neutralizing MAbs could be redirected to HPV6 L1 virus-like particles in which as few as two substitutions of corresponding amino acid residues from HPV11 L1 have been made, thus demonstrating the importance of these residues to MAb binding through the transfer of a conformationally dependent epitope. In addition, a fourth neutralizing MAb could be distinguished from the other neutralizing MAbs in terms of the amino acid residues which affect binding, suggesting the possibility that it neutralizes HPV11 through a different mechanism.
摘要
通过中和抗体对病毒结合进行表征,对于理解病毒感染性的早期事件以及疫苗开发都非常重要。已经描述了针对11型人乳头瘤病毒(HPV11)的中和单克隆抗体(MAb),但由于L1衣壳蛋白上关键的型特异性中和表位具有构象性质,绘制其结合位点一直很困难。我们已经确定了HPV11 L1蛋白中赋予HPV11中和MAb结合型特异性的那些残基。三种HPV11特异性中和MAb的结合可以重定向到HPV6 L1病毒样颗粒上,其中HPV11 L1中相应氨基酸残基的替换少至两个,从而通过构象依赖性表位的转移证明了这些残基对MAb结合的重要性。此外,就影响结合的氨基酸残基而言,第四种中和MAb可以与其他中和MAb区分开来,这表明它可能通过不同机制中和HPV11。
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