序贯包膜免疫诱导 HIV 中和 B 细胞谱系。

Initiation of HIV neutralizing B cell lineages with sequential envelope immunizations.

机构信息

Duke Human Vaccine Institute, Duke University School of Medicine, Durham, NC, 27710, USA.

Boston Children's Hospital and Harvard Medical School, Boston, MA, 02115, USA.

出版信息

Nat Commun. 2017 Nov 23;8(1):1732. doi: 10.1038/s41467-017-01336-3.

A strategy for HIV-1 vaccine development is to define envelope (Env) evolution of broadly neutralizing antibodies (bnAbs) in infection and to recreate those events by vaccination. Here, we report host tolerance mechanisms that limit the development of CD4-binding site (CD4bs), HCDR3-binder bnAbs via sequential HIV-1 Env vaccination. Vaccine-induced macaque CD4bs antibodies neutralize 7% of HIV-1 strains, recognize open Env trimers, and accumulate relatively modest somatic mutations. In naive CD4bs, unmutated common ancestor knock-in mice EnvB cell clones develop anergy and partial deletion at the transitional to mature B cell stage, but become Env upon receptor editing. In comparison with repetitive Env immunizations, sequential Env administration rescue anergic Env (non-edited) precursor B cells. Thus, stepwise immunization initiates CD4bs-bnAb responses, but immune tolerance mechanisms restrict their development, suggesting that sequential immunogen-based vaccine regimens will likely need to incorporate strategies to expand bnAb precursor pools.

一种 HIV-1 疫苗开发策略是在感染过程中定义广泛中和抗体（bnAb）的包膜（Env）进化，并通过接种疫苗来重现这些事件。在这里，我们报告了宿主耐受机制，该机制通过连续的 HIV-1 Env 疫苗接种限制了 CD4 结合位点（CD4bs）和 HCDR3 结合 bnAb 的发展。疫苗诱导的猕猴 CD4bs 抗体中和了 7%的 HIV-1 株，识别开放的 Env 三聚体，并积累了相对适度的体细胞突变。在未突变的 CD4bs 中，未突变的共同祖先敲入小鼠 EnvB 细胞克隆在过渡到成熟 B 细胞阶段时会产生失能和部分缺失，但在受体编辑后会成为 Env。与重复的 Env 免疫相比，连续的 Env 给药可挽救失能的 Env（未编辑）前体 B 细胞。因此，逐步免疫会引发 CD4bs-bnAb 反应，但免疫耐受机制限制了它们的发展，这表明基于免疫原的序贯免疫接种方案可能需要纳入扩大 bnAb 前体池的策略。