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高比例的抗肽抗体可识别口蹄疫病毒颗粒。

A high proportion of anti-peptide antibodies recognize foot-and-mouth disease virus particles.

作者信息

Parry N R, Syred A, Rowlands D J, Brown F

机构信息

Wellcome Biotech, Beckenham, Kent, U.K.

出版信息

Immunology. 1988 Aug;64(4):567-72.

Abstract

Synthetic peptides representing the amino acid sequence 141-160 of the structural protein VP1 of foot-and-mouth disease virus (FMDV) elicit virus-neutralizing antibody. Absorption of anti-peptide sera with purified virus particles removed all detectable virus-binding and neutralizing activity, and reduced the ELISA titres against the homologous peptide by 31-41%. The proportion of anti-peptide antibodies that also recognized virus was unaffected by whether the peptide had been inoculated free, carrier-linked or as part of a fusion protein. The majority of these antibodies reacted with sites composed of residues 142-150. Peptides extended at the amino terminus, into regions shown to be poorly antigenic on the intact virus, induced greater neutralizing responses by increasing the proportion of virus-binding antibodies recognizing region 141-150 from 35% to 70%. However, the total proportion of activity against the longer homologous peptide removed by virus absorption remained within the range 31-41%.

摘要

代表口蹄疫病毒(FMDV)结构蛋白VP1氨基酸序列141 - 160的合成肽可引发病毒中和抗体。用纯化的病毒颗粒吸收抗肽血清可去除所有可检测到的病毒结合和中和活性,并使针对同源肽的ELISA效价降低31 - 41%。抗肽抗体中也识别病毒的比例不受肽是以游离形式、与载体连接还是作为融合蛋白的一部分进行接种的影响。这些抗体中的大多数与由残基142 - 150组成的位点发生反应。在氨基末端延伸至完整病毒上显示抗原性较差区域的肽,通过将识别区域141 - 150的病毒结合抗体比例从35%提高到70%,诱导出更强的中和反应。然而,被病毒吸收去除的针对较长同源肽的活性总比例仍保持在31 - 41%的范围内。

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