Alteration of immunogenicity and antibody recognition of B-cell epitopes by synthetic branched chain polypeptide carriers with poly[L-lysine] backbone.

F Hudecz
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Abstract

In order to elucidate structural and biological properties required for an optimal immunological carrier function and to provide a rational basis for its selection, two new groups of synthetic branched polypeptides with a general formula poly[Lys-(X(i)-DL-Ala(m))][XAK] or poly[Lys-(DL-Ala(m)-X(i))][AXK], where m approximately 3 and i < 1 were introduced by our laboratory. Here we review our recent results on the application of these polypeptides as biodegradable carriers for constructing synthetic immunogens/antigens with a well-known phenyl oxazolone hapten, peptide epitopes of epithelial mucin [MUCI] or herpes simplex virus [HSV 1] glycoprotein D. Observations collected during the last five years with the conjugates presented serve to illustrate the usefulness of branched polypeptides as carriers for the rational design of synthetic immunogens for the development of vaccines or clinically relevant immunodiagnostics. Furthermore, this polypeptide model system enables the analysis and potentially reliable interpretation of the correlation between chemical structure and immunogenic/antigenic features.

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合成聚赖氨酸支链多肽载体对b细胞表位免疫原性和抗体识别的影响。
为了阐明最佳免疫载体功能所需的结构和生物学特性,并为其选择提供合理依据,我们实验室引入了两组新的合成支链多肽,其通式为poly[Lys-(X(i)-DL-Ala(m))][XAK]或poly[Lys-(DL-Ala(m)-X(i))][AXK],其中m近似于3,i < 1。本文综述了近年来这些多肽作为可生物降解载体在构建含苯恶唑酮半抗原的合成免疫原/抗原中的应用。上皮黏液蛋白(MUCI)或单纯疱疹病毒(HSV 1)糖蛋白的肽表位D.在过去五年中所收集到的结合物的观察结果表明,支化多肽作为载体对于合理设计合成免疫原以开发疫苗或临床相关的免疫诊断是有用的。此外,该多肽模型系统能够分析和潜在可靠地解释化学结构与免疫原性/抗原性特征之间的相关性。
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