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Elicitation of HIV-1-neutralizing antibodies against the CD4-binding site

机译:引发针对CD4结合位点的HIV-1中和抗体

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Purpose of Review: The HIV-1 site of binding for the CD4 receptor has long attracted attention as a potential supersite of vulnerability to antibody-mediated neutralization. We review recent findings related to effective CD4-binding site antibodies isolated from HIV-1-infected individuals and discuss implications for immunogen design. Recent Findings: Highly effective CD4-binding site antibodies such as antibody VRC01 have the ability to neutralize over 90% of circulating HIV-1 strains. Sequence and structural analysis of these antibodies from over half a dozen HIV-1-infected donors reveals remarkable similarity in their ontogenies and their modes of recognition, all of which involve mimicry of CD4 receptor by antibody-heavy chain. Meanwhile, other effective CD4-binding site neutralizers such as antibody CH103 have been shown to utilize a different mode of recognition, with next-generation sequencing of both virus and antibody suggesting co-evolution to drive the development of antibody-neutralization breadth. Summary: The nexus of information concerning the CD4-binding site and its recognition by human antibodies capable of effective neutralization has expanded remarkably in the last few years. Although barriers are substantial, new insights from donor-serum responses, atomic-level structures of antibody-Env complexes, and next-generation sequencing of B-cell transcripts are invigorating vaccine-design efforts to elicit effective CD4-binding site antibodies.
机译:审查目的:与CD4受体结合的HIV-1位点作为抗体介导的中和作用的潜在潜在超级位点,早已引起人们的关注。我们回顾了与从HIV-1感染者分离的有效CD4结合位点抗体相关的最新发现,并讨论了对免疫原设计的影响。最新发现:高效的CD4结合位点抗体(例如VRC01抗体)具有中和超过90%的循环HIV-1毒株的能力。来自超过六名感染HIV-1的供体的这些抗体的序列和结构分析表明,它们的本体和识别方式具有显着相似性,所有这些都涉及抗体重链模拟CD4受体。同时,其他有效的CD4结合位点中和剂(例如抗体CH103)已显示出利用不同的识别方式,病毒和抗体的下一代测序表明共同进化可以推动抗体中和广度的发展。简介:在过去的几年中,有关CD4结合位点及其被能够有效中和的人抗体识别的信息的联系已显着扩展。尽管障碍很大,但来自供体血清反应,抗体-Env复合物的原子级结构以及B细胞转录物的下一代测序的新见识正在激发疫苗设计工作,以激发有效的CD4结合位点抗体。

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