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Ephedrine enhances HIV-1 reactivation from latency through elevating tumor necrosis factor receptor II (TNFRII) expression

机译:麻黄碱通过提高肿瘤坏死因子受体II(TNFRII)的表达来增强HIV-1从潜伏期的重新激活。

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摘要

HIV-1 persists during antiretroviral therapy (ART) due to long-lived and proliferating latently-infected host cells, with the outcome being an incomplete cure. The latently-infected cells, or reservoir cells, are transcriptionally absent and invisible to the immune response. Elimination of latency is one strategy in activating virus production, making it visible to immune clearance. We previously showed that Ephedrae herba reactivated HIV-1 from latency. In this study, we used ephedrine, a major component of Ephedra herba, to reactivate HIV-1 from latency. The results showed that ephedrine enhances HIV-1 reactivation in the presence of TNFα. Combination treatment demonstrates a synergistic effect of HIV-1 reactivation compared to TNFα alone. Ephedrine treatment shows a higher TNFRII expression level, which is related to increased HIV-1 reactivation. However, the mechanism of ephedrine in HIV-1 reactivation is still unclear, and may be related to TNFRII receptor expression. Our results indicate that ephedrine enhances HIV-1 reactivation from latency in combination with TNFα treatment. This new reagent could be a promising latency reversal agent (LRA).
机译:HIV-1在抗逆转录病毒疗法(ART)期间由于长期感染和潜伏感染的宿主细胞的增殖而持续存在,其结果是无法完全治愈。潜在感染的细胞或储库细胞在转录上不存在,并且对免疫反应不可见。消除潜伏期是激活病毒产生并使免疫清除可见的一种策略。我们之前的研究表明,麻黄药草可从潜伏期重新激活HIV-1。在这项研究中,我们使用麻黄碱(麻黄的主要成分)从潜伏期重新激活HIV-1。结果表明,在存在TNFα的情况下,麻黄碱可增强HIV-1的活化。与单独的TNFα相比,联合治疗显示HIV-1激活具有协同作用。麻黄碱治疗显示较高的TNFRII表达水平,这与增加的HIV-1活化有关。但是,麻黄碱在HIV-1激活中的机制仍不清楚,可能与TNFRII受体表达有关。我们的结果表明,麻黄碱与TNFα治疗相结合,可提高潜伏期的HIV-1激活。这种新试剂可能是有前途的潜伏时间逆转剂(LRA)。

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