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Focused evolution of HIV-1 neutralizing antibodies revealed by crystal structures and deep sequencing

机译:晶体结构和深度测序揭示了HIV-1中和抗体的聚焦进化

摘要

Antibody VRC01 represents a human immunoglobulin that neutralizes—˜90% of diverse HIV-1 isolates. To understand how such broadly neutralizing HIV-1 antibodies develop and recognize the viral envelope, we used X-ray crystallography and 454 pyrosequencing to characterize additional antibodies from HIV-1-infected individuals. Crystal structures revealed a convergent mode of binding of different antibodies to the same CD4-binding-site epitope. Antibody recognition was achieved through the evolution of complementary contact domains that were generated in diverse ways. Phylogenetic analysis of expressed heavy and light chains determined by deep sequencing revealed a common pathway of antibody heavy chain maturation confined to IGHV1-2*02 lineage that could pair with different light chains. The maturation pathway inferred by antibodyomics reveals that diverse antibodies evolve to a highly affinity-matured state to recognize an invariant viral structure, providing insight into the development and evolution of broadly neutralizing HIV-1 immunity.
机译:抗体VRC01代表中和的人免疫球蛋白,约占90%的各种HIV-1分离物。为了了解这种广泛中和的HIV-1抗体如何发展并识别病毒包膜,我们使用了X射线晶体学和454焦磷酸测序来表征来自HIV-1感染者的其他抗体。晶体结构揭示了不同抗体与相同CD4结合位点表位结合的收敛模式。通过以多种方式产生的互补接触域的进化来实现抗体识别。通过深测序确定表达的重链和轻链的系统发育分析显示,抗体重链成熟的常见途径仅限于IGHV1-2 * 02谱系,可以与不同的轻链配对。通过抗体组学推断出的成熟途径表明,多种抗体进化为高度亲和力成熟的状态,以识别不变的病毒结构,从而为广泛中和HIV-1免疫的发展和进化提供了见识。

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