Multi-Parameter Exploration of HIV-1 Virus-Like Particles as Neutralizing Antibody Immunogens in Guinea Pigs, Rabbits and Macaques.

Tommy Tong, Ema T Crooks, Keiko Osawa, James E Robinson, Mary Barnes, Cristian Apetrei, James M Binley
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Abstract

Virus-like particles (VLPs) offer a platform to test the hypothesis that, since antibody binding to native envelope glycoprotein (Env) trimers results in HIV-1 neutralization, that native Env trimers presented in membranes may be useful for inducing neutralizing antibodies (nAbs) in a vaccine setting. So far, VLPs have not fulfilled this potential. Here, using a "shotgun" approach, we evaluated a wide cross-section of variables in a series of VLP immunizations. We identified 3 tentative leads. First, that VLP doses may not have been sufficient for optimal nAb induction. Second, that dampening the antigenicity of non-functional Env (for example uncleaved gp160) using either protease digests or IgG masking may be useful. Third, that guinea pig sera preferentially target non-conserved epitopes and exhibit relatively high background activity, suggesting that rabbits may be preferable as small animal vaccine models. Recent immunogenicity studies in rabbits appear to bear out all 3 of these leads.

在豚鼠、家兔和猕猴体内作为中和抗体免疫原的 HIV-1 病毒样颗粒的多参数探索。
由于抗体与原生包膜糖蛋白(Env)三聚体结合会导致 HIV-1 中和,因此膜中的原生 Env 三聚体可能有助于在疫苗环境中诱导中和抗体(nAbs)。到目前为止,VLPs 还没有发挥出这种潜力。在此,我们采用 "散弹枪 "方法,对一系列 VLP 免疫中的各种变量进行了评估。我们发现了三条初步线索。首先,VLP 的剂量可能不足以诱导出最佳的 nAb。其次,使用蛋白酶消化法或 IgG 屏蔽法抑制无功能 Env(例如未水解的 gp160)的抗原性可能有用。第三,豚鼠血清优先靶向非保留表位,并表现出相对较高的背景活性,这表明兔子可能更适合作为小动物疫苗模型。最近在兔子身上进行的免疫原性研究似乎证实了上述 3 条线索。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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