利用免疫细胞消除艾滋病病毒库。

Current opinion in HIV and AIDS Pub Date : 2024-03-01 Epub Date: 2024-01-02 DOI:10.1097/COH.0000000000000840
Paula Grasberger, Abigail R Sondrini, Kiera L Clayton
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摘要

综述的目的:尽管数十年来人们对 CD8+ T 细胞和自然杀伤(NK)细胞如何促进感染的自然控制有了深入的了解,但要开发出治疗方法,还需要克服更多的障碍(细胞免疫的突变逃逸、序列多样性和难以获得的组织库)。在这篇综述中,我们将重点介绍抗病毒细胞免疫新机制的最新发现,并讨论当前的治疗策略:值得注意的是,病毒抗原特异性的 MHC-E 限制性 CD8+ T 细胞和 NK 细胞、白细胞介素 (IL)-15 生物制剂在增强细胞毒性方面的作用,以及广谱中和抗体以其原生形式或作为抗体片段在中和病毒和调动细胞免疫力方面的作用明显趋同。最后,髓系细胞作为相关病毒库再次引起人们的关注,这对于设计包容性治疗策略来说是一个令人鼓舞的迹象。摘要:多项研究表明,许多临床前疾病模型都很有希望,包括非人灵长类动物的猿猴免疫缺陷病毒(SIV)/SHIV 感染和人源化小鼠的 HIV 感染。然而,每种模型都有其自身的局限性,可能无法完全预测人类的反应。我们急切地等待着临床试验的结果,评估这些策略对减少病毒库、延缓病毒反弹或最终在不使用联合抗逆转录病毒疗法(cART)的情况下通过免疫控制感染的疗效。
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Harnessing immune cells to eliminate HIV reservoirs.

Purpose of review: Despite decades of insights about how CD8 + T cells and natural killer (NK) cells contribute to natural control of infection, additional hurdles (mutational escape from cellular immunity, sequence diversity, and hard-to-access tissue reservoirs) will need to be overcome to develop a cure. In this review, we highlight recent findings of novel mechanisms of antiviral cellular immunity and discuss current strategies for therapeutic deisgn.

Recent findings: Of note are the apparent converging roles of viral antigen-specific MHC-E-restricted CD8 + T cells and NK cells, interleukin (IL)-15 biologics to boost cytotoxicity, and broadly neutralizing antibodies in their native form or as anitbody fragments to neutralize virus and engage cellular immunity, respectively. Finally, renewed interest in myeloid cells as relevant viral reservoirs is an encouraging sign for designing inclusive therapeutic strategies.

Summary: Several studies have shown promise in many preclinical models of disease, including simian immunodeficiency virus (SIV)/SHIV infection in nonhuman primates and HIV infection in humanized mice. However, each model comes with its own limitations and may not fully predict human responses. We eagerly await the results of clinical trails assessing the efficacy of these strategies to achieve reductions in viral reservoirs, delay viral rebound, or ultimately elicit immune based control of infection without combination antiretroviral therapy (cART).

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