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Vaccines Targeting PreS1 Domain Overcome Immune Tolerance in HBV Carrier Mice

机译:针对PreS1域的疫苗克服了HBV携带者小鼠的免疫耐受性。

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摘要

Strong tolerance to HBV surface antigens limits the therapeutic effect of the conventional HBsAg vaccination in both preclinical animal models and patients with chronic hepatitis B (CHB) infection. In contrast, we observed that clinical CHB patients presented less immune tolerance to the preS1 domain of HBV large surface antigen. To study whether targeting the weak tolerance of preS1 region could improve therapy gain, we explored vaccination with the long peptide of preS1 domain for HBV virions clearance. Our study showed that this preS1-polypeptide rather than HBsAg vaccination induced robust immune responses in the HBV carrier mice. The anti-preS1 rapidly cleared HBV virions in vivo and blocked HBV infection to hepatocytes in vitro. Intriguingly, vaccination of preS1-polypeptide even reduced the tolerized status of HBsAg, opening a therapeutic window for the host to respond to the HBsAg vaccine. A sequential administration of antigenically distinct preS1-polypeptide and HBsAg vaccines in HBV carrier mice could finally induce HBsAg-HBsAb serological conversion and clear chronic HBV infection in the carrier mice. These results suggest that preS1 can function as a therapeutic vaccination for the control of CHB.
机译:对HBV表面抗原的强耐受性限制了常规HBsAg疫苗在临床前动物模型和慢性乙型肝炎(CHB)感染患者中的治疗效果。相反,我们观察到临床CHB患者对HBV大表面抗原的preS1结构域的免疫耐受性较低。为了研究针对preS1区域的弱耐受性能否提高治疗效果,我们探索了用preS1域长肽进行HBV病毒粒子清除的疫苗接种。我们的研究表明,这种preS1多肽而非HBsAg疫苗可在HBV携带者小鼠中诱导强大的免疫反应。抗-preS1可在体内快速清除HBV病毒颗粒,并在体外阻断HBV对肝细胞的感染。有趣的是,preS1多肽的疫苗接种甚至降低了HBsAg的耐受状态,为宿主应对HBsAg疫苗打开了治疗窗口。在HBV携带者小鼠中依次施用抗原性不同的preS1-多肽和HBsAg疫苗最终可以在携带者小鼠中诱导HBsAg-HBsAb血清学转化并清除慢性HBV感染。这些结果表明,preS1可以作为控制CHB的治疗性疫苗。

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