Department of Surgery, Duke University Medical Center, Durham, North Carolina, USA.
UNC HIV Cure Center and.
J Clin Invest. 2020 Oct 1;130(10):5157-5170. doi: 10.1172/JCI135557.
The correlation of HIV-specific antibody-dependent cellular cytotoxicity (ADCC) responses with protection from and delayed progression of HIV-1 infection provides a rationale to leverage ADCC-mediating antibodies for treatment purposes. We evaluated ADCC mediated by different combinations of 2 to 6 neutralizing and non-neutralizing anti-HIV-1 Envelope (Env) mAbs, using concentrations ≤ 1 μg/mL, to identify combinations effective at targeting latent reservoir HIV-1 viruses from 10 individuals. We found that within 2 hours, combinations of 3 mAbs mediated more than 30% killing of HIV-infected primary CD4+ T cells in the presence of autologous NK cells, with the combination of A32 (C1C2), DH511.2K3 (MPER), and PGT121 (V3) mAbs being the most effective. Increasing the incubation of target and effector cells in the presence of mAb combinations from 2 to 24 hours resulted in increased specific killing of infected cells, even with neutralization-resistant viruses. The same combination eliminated reactivated latently HIV-1-infected cells in an ex vivo quantitative viral outgrowth assay. Therefore, administration of a combination of 3 mAbs should be considered in planning in vivo studies seeking to eliminate persistently HIV-1-infected cells.
HIV 特异性抗体依赖的细胞细胞毒性 (ADCC) 反应与 HIV-1 感染的保护和延迟进展相关,这为利用 ADCC 介导的抗体进行治疗提供了依据。我们评估了不同组合的 2 至 6 种中和和非中和抗 HIV-1 包膜 (Env) mAb 介导的 ADCC,使用浓度 ≤ 1 μg/mL,以鉴定能够靶向 10 名个体潜伏储存 HIV-1 病毒的有效组合。我们发现,在 2 小时内,3 种 mAb 的组合在存在自体 NK 细胞的情况下介导了超过 30%的 HIV 感染的原代 CD4+ T 细胞的杀伤,其中 A32 (C1C2)、DH511.2K3 (MPER) 和 PGT121 (V3) mAb 的组合最有效。在 mAb 组合存在的情况下,将靶细胞和效应细胞的孵育时间从 2 小时增加到 24 小时,会导致感染细胞的特异性杀伤增加,即使是对中和耐药的病毒也是如此。相同的组合在体外定量病毒扩增测定中消除了重新激活的潜伏 HIV-1 感染细胞。因此,在计划进行体内研究以消除持续感染 HIV-1 的细胞时,应考虑使用 3 种 mAb 的组合。
