腺相关病毒载体递送HIV生物制品:有望实现HIV感染的“单针”功能性治疗

IF 3.5 4区 医学 Q2 IMMUNOLOGY
Patricia A. Hahn , Mauricio A. Martins
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引用次数: 1

摘要

基于免疫球蛋白的HIV生物制剂(Ig-HIV),包括广泛中和抗体,在临床前和临床研究中抑制病毒复制的能力说明了这些分子如何作为抗逆转录病毒疗法的替代品或佐剂来治疗HIV感染。然而,目前提供Ig-HIV的模式需要反复被动注入,这在大规模实施方面面临着后勤和经济挑战。克服这些障碍并实现Ig-HIV在体内持续表达的一种有希望的方法是利用腺相关病毒(AAV)载体将Ig-HIV基因转移到宿主细胞。由于AAV载体是非致病性的,并且它们的基因组作为附加体存在于细胞核中,因此转基因表达可以持续AAV转导细胞的生命。鉴于肌细胞的寿命长,骨骼肌是基于AAV的免疫疗法的首选组织,旨在实现Ig-HIV的持续递送。与这一观点一致的是,最近的研究表明,一次性肌肉注射AAV/Ig HIV载体可以实现对HIV的终身免疫。然而,实现这种方法的前景面临着重大障碍,包括AAV递送的Ig-HIV诱导抗药物抗体的潜力,以及AAV在人群中的高血清流行率。在这里,我们描述了这些宿主免疫反应如何阻碍AAV/Ig HIV治疗,并回顾了目前克服这些障碍的策略。鉴于AAV/Ig HIV治疗有可能保持无抗逆转录病毒疗法的病毒学抑制,并防止HIV感染者再次感染,优化这一策略应成为HIV/AIDS研究的更优先事项。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Adeno-associated virus-vectored delivery of HIV biologics: the promise of a “single-shot” functional cure for HIV infection

Adeno-associated virus-vectored delivery of HIV biologics: the promise of a “single-shot” functional cure for HIV infection

Adeno-associated virus-vectored delivery of HIV biologics: the promise of a “single-shot” functional cure for HIV infection

The ability of immunoglobulin-based HIV biologics (Ig-HIV), including broadly neutralizing antibodies, to suppress viral replication in pre-clinical and clinical studies illustrates how these molecules can serve as alternatives or adjuncts to antiretroviral therapy for treating HIV infection. However, the current paradigm for delivering Ig-HIVs requires repeated passive infusions, which faces both logistical and economic challenges to broad-scale implementation. One promising way to overcome these obstacles and achieve sustained expression of Ig-HIVs in vivo involves the transfer of Ig-HIV genes to host cells utilizing adeno-associated virus (AAV) vectors. Because AAV vectors are non-pathogenic and their genomes persist in the cell nucleus as episomes, transgene expression can last for as long as the AAV-transduced cell lives. Given the long lifespan of myocytes, skeletal muscle is a preferred tissue for AAV-based immunotherapies aimed at achieving persistent delivery of Ig-HIVs. Consistent with this idea, recent studies suggest that lifelong immunity against HIV can be achieved from a one-time intramuscular dose of AAV/Ig-HIV vectors. However, realizing the promise of this approach faces significant hurdles, including the potential of AAV-delivered Ig-HIVs to induce anti-drug antibodies and the high AAV seroprevalence in the human population. Here we describe how these host immune responses can hinder AAV/Ig-HIV therapies and review current strategies for overcoming these barriers. Given the potential of AAV/Ig-HIV therapy to maintain ART-free virologic suppression and prevent HIV reinfection in people living with HIV, optimizing this strategy should become a greater priority in HIV/AIDS research.

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来源期刊
Journal of Virus Eradication
Journal of Virus Eradication Medicine-Public Health, Environmental and Occupational Health
CiteScore
6.10
自引率
1.80%
发文量
28
审稿时长
39 weeks
期刊介绍: The Journal of Virus Eradication aims to provide a specialist, open-access forum to publish work in the rapidly developing field of virus eradication. The Journal covers all human viruses, in the context of new therapeutic strategies, as well as societal eradication of viral infections with preventive interventions. The Journal is aimed at the international community involved in the prevention and management of viral infections. It provides an academic forum for the publication of original research into viral reservoirs, viral persistence and virus eradication and ultimately development of cures. The Journal not only publishes original research, but provides an opportunity for opinions, reviews, case studies and comments on the published literature. It focusses on evidence-based medicine as the major thrust in the successful management of viral infections.The Journal encompasses virological, immunological, epidemiological, modelling, pharmacological, pre-clinical and in vitro, as well as clinical, data including but not limited to drugs, immunotherapy and gene therapy. It is an important source of information on the development of vaccine programs and preventative measures aimed at virus eradication.
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