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高甘露糖型寡糖和合成寡甘露糖簇与人抗体2G12的结合:对HIV-1疫苗设计的启示

Binding of high-mannose-type oligosaccharides and synthetic oligomannose clusters to human antibody 2G12: implications for HIV-1 vaccine design.

作者信息

Wang Lai-Xi, Ni Jiahong, Singh Suddham, Li Hengguang

机构信息

Institute of Human Virology, University of Maryland Biotechnology Institute, University of Maryland, Baltimore, Maryland 21201, USA.

出版信息

Chem Biol. 2004 Jan;11(1):127-34. doi: 10.1016/j.chembiol.2003.12.020.

Abstract

Human antibody 2G12 broadly neutralizes human immunodeficiency virus type 1 (HIV-1) isolates and shows protective activity against viral challenge in animal models. Previous mutational analysis suggested that 2G12 recognized a novel cluster of high-mannose type oligosaccharides on HIV-1 gp120. To explore the carbohydrate antigen for HIV-1 vaccine design, we have studied the binding of 2G12 to an array of HIV-1 high-mannose type oligosaccharides by competitive ELISAs and found that Man9GlcNAc is 210- and 74-fold more effective than Man5GlcNAc and Man6GlcNAc in binding to 2G12. The results establish that the larger high-mannose oligosaccharide on HIV-1 is the favorable subunit for 2G12 recognition. To mimic the putative epitope of 2G12, we have created scaffold-based multivalent Man9 clusters and found that the galactose-scaffolded bi-, tri-, and tetra-valent Man9 clusters are 7-, 22-, and 73-fold more effective in binding to 2G12 than the monomeric Man9GlcNAc2Asn. The experimental data shed light on further structural optimization of epitope mimics for developing a carbohydrate-based HIV-1 vaccine.

摘要

人源抗体2G12可广泛中和1型人类免疫缺陷病毒(HIV-1)毒株,并在动物模型中显示出对病毒攻击的保护活性。先前的突变分析表明,2G12识别HIV-1 gp120上一组新的高甘露糖型寡糖。为了探索用于HIV-1疫苗设计的碳水化合物抗原,我们通过竞争性酶联免疫吸附测定研究了2G12与一系列HIV-1高甘露糖型寡糖的结合,发现Man9GlcNAc与2G12结合的效率比Man5GlcNAc和Man6GlcNAc分别高210倍和74倍。结果表明,HIV-1上较大的高甘露糖寡糖是2G12识别的有利亚基。为了模拟2G12的推定表位,我们构建了基于支架的多价Man9簇,发现半乳糖支架的二价、三价和四价Man9簇与2G12结合的效率分别比单体Man9GlcNAc2Asn高7倍、22倍和73倍。实验数据为开发基于碳水化合物的HIV-1疫苗的表位模拟物的进一步结构优化提供了线索。

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