Characterization of IL-21-expressing recombinant hepatitis B virus (HBV) as a therapeutic agent targeting persisting HBV infection

Zhongliang Shen; Jingwen Wu; Zixiang Gao; Jingyu Wang; Haoxiang Zhu; Richen Mao; Xuanyi Wang; Jiming Zhang; Youhua Xie; Jing Liu

摘要

Chronic infection by hepatitis B virus (HBV) is associated with high risks of liver fibrosis, cirrhosis and hepatocellular carcinoma. In mouse models of HBV persistence, interleukin 21 (IL-21) has been identified as a potent inducer of viral clearance. Strict hepatotropism makes recombinant HBV (rHBV) vectors ideal for liver-targeting gene delivery. Previously, we established an rHBV vector termed 5c3c, which is highly replicative by itself, but requires HBV envelope proteins provided in trans to produce virions. 5c3c-based rHBV virions are capable of delivering cargo gene expression driven by HBV Sp1 promoter into infected hepatocytes. In this work, we explore the feasibility of using 5c3c-derived rHBV for liver-specific delivery of IL-21 as treatment of chronic HBV infection. Methods: 5c3c-derived rHBV replicons harboring mouse or human IL-21 genes (termed 5c3c-mIL-21 and 5c3c-hIL-21 respectively) were constructed and then tested for the production of rHBV virions in vitro and in vivo. 5c3c-mIL-21's anti-HBV effects were determined in chronic HBV mouse model. Furthermore, superinfection by rHBV virions was analysed using HBV-infected HepG2/NTCP cells and human liver chimeric mice. Results: 5c3c-mIL-21 and 5c3c-hIL-21 were efficiently replicative and produced enveloped virions when provided with envelope proteins, both in vitro and in vivo. In mouse model of HBV persistence, IL-21 expressed from injected 5c3c-mIL-21 replicon induced complete viral clearance. 5c3c-mIL-21 and 5c3c-hIL-21 virions could infect HepG2/NTCP cells and engender sustained IL-21 expression. Most importantly, IL-21-expressing rHBV virions could superinfect HBV-infected HepG2/NTCP cells and human hepatocytes in human liver chimeric mice, and engender sustained IL-21 expression and rHBV production. Conclusion: These data suggest the high potential of 5c3c-derived IL-21-expressing rHBV as a novel therapeutic against chronic HBV infection.? The author(s).

机译：乙型肝炎病毒（HBV）的慢性感染与肝纤维化，肝硬化和肝细胞癌的高风险有关。在HBV持久性的小鼠模型中，白细胞介素21（IL-21）已被鉴定为病毒间隙的有效诱导剂。严格的肝细胞使重组HBV（RHBV）载体是理想的肝靶向基因递送。以前，我们建立了一种rhBV载体，其称为5C3C，其自身具有高度复制，但需要在反式中提供HBV包膜蛋白来产生病毒素。基于5C3C的RHBV病毒藻能够将由HBV SP1启动子驱动的货物基因表达输送到受感染的肝细胞中。在这项工作中，我们探讨了使用5C3C衍生的RHBV进行IL-21特定肝脏递送的可行性作为慢性HBV感染的治疗方法。方法：构建含小鼠或人IL-21基因（分别称为5C3C-MIL-21和5C3C-HIL-21的5C3C衍生的RHBV复制子，然后在体外和体内测试RHBV病毒藻。在慢性HBV小鼠模型中测定5C3C-MIL-21的抗HBV效应。此外，使用HBV感染的HepG2 / NTCP细胞和人肝嵌合小鼠分析RHBV病毒藻的SuperInfection。结果：5C3C-MIL-21和5C3C-HIL-21当在体外和体内提供包封蛋白时，有效复制和产生包膜病毒。在HBV持久性的小鼠模型中，IL-21从注射的5C3C-MIL-21复制品诱导完全病毒间隙。 5C3C-MIL-21和5C3C-HIL-21病毒粒子可以感染HepG2 / NTCP细胞并发芽持续的IL-21表达。最重要的是，IL-21表达的RHBV病毒群体可以使HBV感染的HEPG2 / NTCP细胞和人肝细胞中的人肝嵌合小鼠，并获得持续的IL-21表达和RHBV产生。结论：这些数据表明5C3C衍生的IL-21表达rhBV的高潜力作为一种针对慢性HBV感染的新疗法。作者。

Characterization of IL-21-expressing recombinant hepatitis B virus (HBV) as a therapeutic agent targeting persisting HBV infection

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