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Therapeutic vaccines in HBV: lessons from HCV

机译:乙肝病毒治疗疫苗:丙肝病毒的经验教训

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Currently, millions of people infected with hepatitis B virus (HBV) are committed to decades of treatment with anti-viral therapy to control viral replication. However, new tools for immunotherapy that include both viral vectors and molecular checkpoint inhibitors are now available. This has led to a resurgence of interest in new strategies to develop immunotherapeutic strategies with the aim of inducing HBeAg seroconversion-an end-point that has been associated with a decrease in the rates of disease progression. Ultimately, a true cure will involve the elimination of covalently closed circular DNA which presents a greater challenge for immunotherapy. In this manuscript, I describe the development of immunotherapeutic strategies for HBV that are approaching or currently in clinical studies, and draw on observations of T cell function in natural infection supported by recent animal studies that may lead to additional rational vaccine strategies using checkpoint inhibitors. I also draw on our recent experience in developing potent vaccines for HCV prophylaxis based on simian adenoviral and MVA vectors used in prime-boost strategies in both healthy volunteers and HCV infected patients. I have shown that the induction of T cell immune responses is markedly attenuated when administered to people with persistent HCV viremia. These studies and recently published animal studies using the woodchuck model suggest that potent vaccines based on DNA or adenoviral vectored vaccination represent a rational way forward. However, combining these with drugs to suppress viral replication, alongside checkpoint inhibitors may be required to induce long-term immune control.
机译:目前,数百万感染了乙型肝炎病毒(HBV)的人致力于使用抗病毒疗法控制病毒复制数十年。但是,现在可以使用包括病毒载体和分子检查点抑制剂的新型免疫疗法工具。这导致人们对开发免疫治疗策略的新策略重新产生兴趣,该策略旨在诱导HBeAg血清转化-这是与疾病进展速度降低相关的终点。最终,真正的治疗将涉及消除共价闭合的环状DNA,这对免疫疗法提出了更大的挑战。在本手稿中,我描述了正在或正在临床研究中的针对HBV的免疫治疗策略的发展,并借鉴了最近动物研究支持的自然感染中T细胞功能的观察结果,这些结果可能导致使用检查点抑制剂的其他合理疫苗策略。我还将借鉴我们最近在健康志愿者和HCV感染患者中基于用于加强免疫策略的猿猴腺病毒和MVA载体开发有效的HCV预防疫苗的经验。我已经证明,向患有持续性HCV病毒血症的人服用时,T细胞免疫反应的诱导作用明显减弱。这些研究和最近发表的使用土拨鼠模型的动物研究表明,基于DNA或腺病毒载体接种的有效疫苗代表了一种合理的发展方向。但是,将它们与药物结合以抑制病毒复制,同时可能需要检查点抑制剂来诱导长期免疫控制。

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