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多供体分析揭示了 VRC01 类抗体中和 HIV-1 的结构要素、遗传决定因素和成熟途径。

Multidonor analysis reveals structural elements, genetic determinants, and maturation pathway for HIV-1 neutralization by VRC01-class antibodies.

机构信息

Vaccine Research Center, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Immunity. 2013 Aug 22;39(2):245-58. doi: 10.1016/j.immuni.2013.04.012. Epub 2013 Aug 1.

Abstract

Antibodies of the VRC01 class neutralize HIV-1, arise in diverse HIV-1-infected donors, and are potential templates for an effective HIV-1 vaccine. However, the stochastic processes that generate repertoires in each individual of >10(12) antibodies make elicitation of specific antibodies uncertain. Here we determine the ontogeny of the VRC01 class by crystallography and next-generation sequencing. Despite antibody-sequence differences exceeding 50%, antibody-gp120 cocrystal structures reveal VRC01-class recognition to be remarkably similar. B cell transcripts indicate that VRC01-class antibodies require few specific genetic elements, suggesting that naive-B cells with VRC01-class features are generated regularly by recombination. Virtually all of these fail to mature, however, with only a few-likely one-ancestor B cell expanding to form a VRC01-class lineage in each donor. Developmental similarities in multiple donors thus reveal the generation of VRC01-class antibodies to be reproducible in principle, thereby providing a framework for attempts to elicit similar antibodies in the general population.

摘要

VRC01 类抗体可中和 HIV-1,在不同的 HIV-1 感染供体中产生,是有效 HIV-1 疫苗的潜在模板。然而,在每个人超过 10^12 个抗体的抗体库中产生的随机过程使得特异性抗体的诱导变得不确定。通过结晶学和下一代测序,我们确定了 VRC01 类抗体的发生过程。尽管抗体序列差异超过 50%,但抗体-gp120 共晶体结构显示 VRC01 类识别非常相似。B 细胞转录本表明,VRC01 类抗体仅需要少数特定的遗传元件,这表明具有 VRC01 类特征的幼稚 B 细胞通过重组经常产生。然而,这些细胞几乎都不能成熟,只有少数可能的祖细胞 B 细胞在每个供体中扩展形成 VRC01 类谱系。因此,多个供体的发育相似性揭示了 VRC01 类抗体的产生原则上是可重复的,从而为在普通人群中诱导类似抗体的尝试提供了框架。

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