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Glycosylation Patterns of HIV-1 gp120 Depend on the Type of Expressing Cells and Affect Antibody Recognition*

机译:HIV-1 gp120的糖基化模式取决于表达细胞的类型并影响抗体识别*

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摘要

Human immunodeficiency virus type 1 (HIV-1) entry is mediated by the interaction between a variably glycosylated envelope glycoprotein (gp120) and host-cell receptors. Approximately half of the molecular mass of gp120 is contributed by N-glycans, which serve as potential epitopes and may shield gp120 from immune recognition. The role of gp120 glycans in the host immune response to HIV-1 has not been comprehensively studied at the molecular level. We developed a new approach to characterize cell-specific gp120 glycosylation, the regulation of glycosylation, and the effect of variable glycosylation on antibody reactivity. A model oligomeric gp120 was expressed in different cell types, including cell lines that represent host-infected cells or cells used to produce gp120 for vaccination purposes. N-Glycosylation of gp120 varied, depending on the cell type used for its expression and the metabolic manipulation during expression. The resultant glycosylation included changes in the ratio of high-mannose to complex N-glycans, terminal decoration, and branching. Differential glycosylation of gp120 affected envelope recognition by polyclonal antibodies from the sera of HIV-1-infected subjects. These results indicate that gp120 glycans contribute to antibody reactivity and should be considered in HIV-1 vaccine design.
机译:人类1型免疫缺陷病毒(HIV-1)的进入是由糖基化包膜糖蛋白(gp120)和宿主细胞受体之间的相互作用介导的。 gp120分子质量的大约一半是由N-聚糖贡献的,N-聚糖是潜在的表位,可能使gp120免受免疫识别。 gp120聚糖在宿主对HIV-1的免疫反应中的作用尚未在分子水平上进行全面研究。我们开发了一种新方法来表征细胞特异性gp120糖基化,糖基化的调控以及可变糖基化对抗体反应性的影响。模型寡聚gp120在不同细胞类型中表达,包括代表宿主感染细胞的细胞系或用于疫苗接种目的生产gp120的细胞。 gp120的N-糖基化会有所不同,具体取决于用于其表达的细胞类型和表达过程中的代谢操作。最终的糖基化包括高甘露糖与复杂N-聚糖的比例变化,末端修饰和分支。 gp120的差异糖基化会影响HIV-1感染者血清中的多克隆抗体对包膜的识别。这些结果表明gp120聚糖有助于抗体反应,应在HIV-1疫苗设计中予以考虑。

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