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Clearing Persistent Extracellular Antigen of Hepatitis B Virus: An Immunomodulatory Strategy to Reverse Tolerance for an Effective Therapeutic Vaccination

机译:清除乙型肝炎病毒的持久性细胞外抗原:反向耐受的有效治疗性疫苗免疫调节策略。

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摘要

Development of therapeutic vaccines/strategies to control chronic hepatitis B virus (HBV) infection (CHB) has been challenging due to HBV-induced tolerance. In this study, we explored strategies for breaking tolerance and restoring the immune response to the HBV surface antigen in tolerant mice. We demonstrated that immune tolerance status is attributed to the level and duration of circulating HBsAg in HBV carrier models. Removal of circulating HBsAg by a monoclonal anti-HBsAg antibody in tolerant mice could gradually reduce tolerance and reestablish B cell and CD4+ T cell responses to subsequent Engerix-B vaccination, producing protective IgG. Furthermore, HBsAg-specific CD8+ T cells induced by the addition of a TLR agonist, resulted in clearance of HBV in both serum and liver. Thus, generation of protective immunity can be achieved by clearing extracellular viral antigen with neutralizing antibodies followed by vaccination.
机译:由于HBV诱导的耐受性,控制慢性乙型肝炎病毒(HBV)感染(CHB)的治疗性疫苗/策略的开发一直具有挑战性。在这项研究中,我们探索了在耐受性小鼠中打破耐受性并恢复对HBV表面抗原的免疫反应的策略。我们证明了免疫耐受状态归因于HBV携带者模型中循环HBsAg的水平和持续时间。在耐受性小鼠中通过单克隆抗HBsAg抗体清除循环中的HBsAg可逐渐降低耐受性,并重新建立B细胞和CD4 + T细胞对随后的Engerix-B疫苗的反应,从而产生保护性IgG。此外,通过添加TLR激动剂诱导的HBsAg特异性CD8 + T细胞导致血清和肝脏中的HBV清除。因此,可以通过用中和抗体清除细胞外病毒抗原然后进行疫苗接种来实现保护性免疫的产生。

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