阴道应用中和性和非中和性抑制性抗体对猕猴阴道 SHIV 挑战的保护作用。
Protective effect of vaginal application of neutralizing and nonneutralizing inhibitory antibodies against vaginal SHIV challenge in macaques.
机构信息
U1110 INSERM/UNISTRA, Institute of Virology, Strasbourg, France.
1] CEA, Division of Immuno-Virology, iMETI, DSV, Fontenay-aux-Roses, France [2] UMR-E1, Université Paris Sud-11, Orsay, France.
出版信息
Mucosal Immunol. 2014 Jan;7(1):46-56. doi: 10.1038/mi.2013.23. Epub 2013 Apr 17.
Definition of antibody (Ab) functions capable of preventing mucosal HIV transmission may be critical to both effective vaccine development and the prophylactic use of monoclonal Abs. Although direct antibody-mediated neutralization is highly effective against cell-free virus, increasing evidence suggests an important role for immunoglobulin G (IgG) Fcγ receptor (FcγR)-mediated inhibition of HIV replication. Thus, a panel of well-known neutralizing (NAbs) and nonneutralizing Abs (NoNAbs) were screened for their ability to block HIV acquisition and replication in vitro in either an independent or FcγR-dependent manner. Abs displaying the highest Fc-mediated inhibitory activity in various in vitro assays were selected, formulated for topical vaginal application in a microbicide gel, and tested for their antiviral activity against SHIVSF162P3 vaginal challenge in non-human primates (NHPs). A combination of three NAbs, 2G12, 2F5, and 4E10, fully prevented simian/human immunodeficiency virus (SHIV) vaginal transmission in 10 out of 15 treated NHPs, whereas a combination of two NoNAbs, 246-D and 4B3, although having no impact on SHIV acquisition, reduced plasma viral load. These results indicate that anti-HIV Abs with distinct neutralization and inhibitory functions differentially affect in vivo HIV acquisition and replication, by interfering with early viral replication and dissemination. Therefore, combining diverse Ab properties may potentiate the protective effects of anti-HIV-Ab-based strategies.
抗体(Ab)功能的定义,这些功能能够预防黏膜 HIV 传播,这对于有效疫苗的开发和单克隆抗体的预防性使用可能至关重要。虽然直接的抗体介导的中和作用对游离病毒非常有效,但越来越多的证据表明免疫球蛋白 G(IgG)Fcγ 受体(FcγR)介导的抑制 HIV 复制的作用非常重要。因此,筛选了一组众所周知的中和(NAb)和非中和(NoNAb)抗体,以研究它们是否能够以独立或 FcγR 依赖的方式在体外阻断 HIV 的获得和复制。筛选出在各种体外测定中显示出最高 Fc 介导抑制活性的抗体,将其配制成杀微生物剂凝胶的局部阴道应用,并在非人类灵长类动物(NHP)中测试其针对 SHIVSF162P3 阴道挑战的抗病毒活性。三种 NAb(2G12、2F5 和 4E10)的组合完全阻止了 15 只接受治疗的 NHP 中的 10 只发生猴免疫缺陷病毒(SHIV)阴道传播,而两种 NoNAb(246-D 和 4B3)的组合虽然对 SHIV 的获得没有影响,但降低了血浆病毒载量。这些结果表明,具有不同中和和抑制功能的抗 HIV 抗体通过干扰早期病毒复制和传播,不同程度地影响体内 HIV 的获得和复制。因此,结合不同的 Ab 特性可能增强基于抗 HIV-Ab 策略的保护作用。
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