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Envelope-specific antibodies and antibody-derived molecules for treating and curing HIV infection

机译:信封特异性抗体和抗体衍生的分子用于治疗和治愈HIV感染

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摘要

HIV-1 is a retrovirus that integrates into host chromatin and can remain transcriptionally quiescent in a pool of immune cells. This characteristic enables HIV-1 to evade both host immune responses and antiretroviral drugs, leading to persistent infection. Upon reactivation of proviral gene expression, HIV-1 envelope (HIV-1 Env) glycoproteins are expressed on the cell surface, transforming latently infected cells into targets for HIV-1 Env-specific monoclonal antibodies (mAbs), which can engage immune effector cells to kill productively infected CD4+ T cells and thus limit the spread of progeny virus. Recent innovations in antibody engineering have resulted in novel immunotherapeutics such as bispecific dual-affinity re-targeting (DART) molecules and other bi- and trispecific antibody designs that can recognize HIV-1 Env and recruit cytotoxic effector cells to kill CD4+ T cells latently infected with HIV‑1. Here, we review these immunotherapies, which are designed with the goal of curing HIV-1 infection.
机译:HIV-1是一种逆转录病毒,整合到宿主染色质中,可以在免疫细胞池中保持转录静止。此特征使HIV-1能够逃避宿主的免疫反应和抗逆转录病毒药物,从而导致持续感染。重新激活前病毒基因表达后,HIV-1包膜(HIV-1 Env)糖蛋白在细胞表面表达,将潜伏感染的细胞转变为HIV-1 Env特异性单克隆抗体(mAb)的靶标,该抗体可与免疫效应细胞结合杀死生产性感染的CD4 + T细胞,从而限制了子代病毒的传播。抗体工程学方面的最新创新已产生了新颖的免疫疗法,例如双特异性双亲和性重新靶向(DART)分子以及其他双和三特异性抗体设计,可以识别HIV-1 Env并募集细胞毒性效应细胞来杀死CD4 + T细胞被HIV-1潜在感染。在这里,我们审查这些免疫疗法,旨在治愈HIV-1感染的目标。

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