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Insight into HIV-2 latency may disclose strategies for a cure for HIV-1 infection

机译:深入了解HIV-2潜伏期可能会揭示治愈HIV-1感染的策略

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摘要

HIV-1 and HIV-2 originate from two distinct zoonotic transmissions of simian immunodeficiency viruses from primate to human. Although both share similar modes of transmission and can result in the development of AIDS with similar clinical manifestations, HIV-2 infection is generally milder and less likely to progress to AIDS. HIV is currently incurable due to the presence of HIV provirus integrated into the host DNA of long-lived memory cells of the immune system without active replication. As such, the latent virus is immunologically inert and remains insensitive to the administered antiviral drugs targeting active viral replication steps. Recent evidence suggests that persistent HIV replication may occur in anatomical sanctuaries such as the lymphoid tissue due to low drug penetration. At present, different strategies are being evaluated either to completely eradicate the virus from the patient (sterilising cure) or to allow treatment interruption without viral rebound (functional cure). Because HIV-2 is naturally less pathogenic and displays a more latent phenotype than HIV-1, it may represent a valuable model that provides elementary information to cure HIV-1 infection. Insight into the viral and cellular determinants of HIV-2 replication may therefore pave the way for alternative strategies to eradicate HIV-1 or promote viral remission.
机译:HIV-1和HIV-2源自猿猴免疫缺陷病毒从灵长类动物到人的两种不同的人畜共患病传播。尽管两者都具有相似的传播方式,并可能导致具有相似临床表现的艾滋病的发展,但HIV-2感染通常较轻,发展为AIDS的可能性较小。由于存在HIV病毒原体,该病毒原体整合到免疫系统长寿记忆细胞的宿主DNA中而没有主动复制,因此目前无法治愈。因此,潜伏病毒是免疫学惰性的,并且对靶向活性病毒复制步骤的抗病毒药物保持不敏感。最近的证据表明,由于药物的低渗透性,艾滋病毒的持久复制可能会发生在解剖区域,例如淋巴组织中。目前,正在评估不同的策略,以完全消灭患者的病毒(消毒治愈)或允许治疗中断而无病毒反弹(功能治愈)。因为HIV-2的自然致病性比HIV-1低,并且表现出比HIV-1更强的潜在表型,所以它可能代表了一种有价值的模型,可提供治疗HIV-1感染的基本信息。因此,深入了解HIV-2复制的病毒和细胞决定因素可能为消灭HIV-1或促进病毒缓解的替代策略铺平道路。

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