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HIV-1 相关高甘露糖寡糖-CRM197 糖缀合物的制备、表征和免疫原性。

Preparation, characterization and immunogenicity of HIV-1 related high-mannose oligosaccharides-CRM197 glycoconjugates.

机构信息

Novartis Vaccines and Diagnostics, Research Center, Via Fiorentina 1, 53100, Siena, Italy.

出版信息

Glycoconj J. 2010 Jul;27(5):501-13. doi: 10.1007/s10719-010-9295-0. Epub 2010 Jun 4.

Abstract

The dense glycan shield on the surface of human immunodeficiency virus type 1 (HIV-1) gp120 masks conserved protein epitopes and facilitates virus entry via interaction to glycan binding proteins on susceptible host cells. The broadly neutralizing monoclonal antibody 2G12 binds a cluster of high-mannose oligosaccharides on the gp120 subunit of HIV-1 Env protein. This oligomannose epitope is currently being considered for the design of a synthetic vaccine. The cluster nature of the 2G12 epitope suggests that a multivalent antigen presentation is important to develop a carbohydrate-based vaccine candidate. In this work we describe the development of neoglycoconjugates displaying clustered HIV-1 related oligomannose carbohydrates. We exploited flexible polyamidoamine (PAMAM) scaffold to generate four- and eight-valent sugar clusters of HIV-1-related oligomannose antigens Man(4), Man(6) and Man(9). The multivalent presentation of oligomannoses increased the avidity of Man(4) and Man(9) to 2G12. The synthetic glycodendrons were then covalently coupled to the protein carrier CRM(197), formulated with the adjuvant MF59, and used to immunize two animal species. Oligomannose-specific IgG antibodies were generated; however, the antisera failed to recognize recombinant HIV-1 gp120 proteins. We conclude that further structural vaccinology work is needed to identify an antigen presentation that closely matches in vivo the structure of the epitope mapped by 2G12.

摘要

HIV-1 表面密集的糖蛋白外壳掩盖了保守的蛋白表位,并通过与易感宿主细胞上的糖结合蛋白相互作用促进病毒进入。广泛中和的单克隆抗体 2G12 结合 HIV-1 Env 蛋白 gp120 亚基上的一组高甘露糖寡糖。该寡甘露糖表位目前正在考虑用于设计合成疫苗。2G12 表位的簇状性质表明,多价抗原呈递对于开发基于碳水化合物的疫苗候选物很重要。在这项工作中,我们描述了展示簇状 HIV-1 相关寡甘露糖碳水化合物的新型糖缀合物的开发。我们利用灵活的聚酰胺胺 (PAMAM) 支架生成了 HIV-1 相关寡甘露糖抗原 Man(4)、Man(6)和 Man(9)的四价和八价糖簇。寡甘露糖的多价呈递增加了 2G12 对 Man(4)和 Man(9)的亲和力。然后将合成的糖树突通过共价键连接到蛋白载体 CRM(197)上,并用佐剂 MF59 进行配制,并用于免疫两种动物物种。产生了针对寡甘露糖的 IgG 抗体;然而,抗血清未能识别重组 HIV-1 gp120 蛋白。我们得出结论,需要进一步进行结构疫苗学研究,以确定一种抗原呈递方式,该方式与 2G12 映射的表位的体内结构非常匹配。

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