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利用抗肽抗体和VII组单克隆抗体研究单纯疱疹病毒1型糖蛋白D的N端合成肽的结构特性和反应性

Structural properties and reactivity of N-terminal synthetic peptides of herpes simplex virus type 1 glycoprotein D by using antipeptide antibodies and group VII monoclonal antibodies.

作者信息

Bosch D L, Geerligs H J, Weijer W J, Feijlbrief M, Welling G W, Welling-Wester S

机构信息

Laboratorium voor Medische Microbiologie, Rijksuniversiteit Groningen, The Netherlands.

出版信息

J Virol. 1987 Nov;61(11):3607-11. doi: 10.1128/JVI.61.11.3607-3611.1987.

Abstract

To investigate the contribution of individual amino acids to the antigenicity of the N-terminal region of herpes simplex virus type 1 glycoprotein D, a series of 14 overlapping synthetic peptides within residues 1 to 30 were examined for their reactivity with monoclonal antibody LP14 (a group VII monoclonal antibody; in herpes simplex virus mutants resistant to LP14, arginine 16 is substituted by histidine) and two antipeptide antisera (antipeptide 9-21 and antipeptide 1-23). Maximal binding was achieved with peptides 9-21, 10-30, 9-30, and 8-30 and the chymotryptic fragment 9-17 of peptide 9-21, suggesting that a major antigenic site is located within residues 10 through 17. Lysine 10 was shown to be essential for high reactivity, either by binding directly to the antibody molecule or by stabilizing an ordered structure of the peptide. The importance of ordered structure was demonstrated by a decrease in reactivity after sodium dodecyl sulfate treatment of peptides 9-21 and 8-30.

摘要

为了研究单个氨基酸对单纯疱疹病毒1型糖蛋白D N端区域抗原性的贡献,检测了1至30位残基内的一系列14个重叠合成肽与单克隆抗体LP14(VII组单克隆抗体;在对LP14耐药的单纯疱疹病毒突变体中,第16位精氨酸被组氨酸取代)以及两种抗肽抗血清(抗肽9 - 21和抗肽1 - 23)的反应性。肽9 - 21、10 - 30、9 - 30和8 - 30以及肽9 - 21的胰凝乳蛋白酶消化片段9 - 17实现了最大结合,表明主要抗原位点位于10至17位残基内。赖氨酸10被证明对于高反应性至关重要,其方式要么是直接与抗体分子结合,要么是稳定肽的有序结构。通过对肽9 - 21和8 - 30进行十二烷基硫酸钠处理后反应性降低,证明了有序结构的重要性。

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