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In-vitro and in-vivo models for hepatitis B cure research

机译:乙型肝炎治疗研究的体外和体内模型

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Purpose of review Antiviral therapy for chronic hepatitis B infection is rarely curative, thus research in HBV cure strategies is a priority. Drug development and testing has been hampered by the lack of robust cell culture systems and small animal models. This review summarizes existing models for HBV cure research and focuses on recent developments since 2017 until today. Recent findings The field has progressed in the development of cell culture and animal models to study HBV. Although early cell culture systems relied on transfection of HBV genomes in hepatoma cell lines, novel models expressing the entry receptor for HBV are susceptible to infection. Improved culture conditions for primary human hepatocytes, the primary target of HBV, have enabled the screening and validation of novel antivirals. Mouse models grafted with partially humanized livers are suitable for testing viral entry inhibitors or direct acting antivirals, and can be reconstituted with human immune cells to analyze immunotherapies. Other immunocompetent models include mice transduced with HBV genomes or woodchucks infected with their native hepatitis virus. Model systems for HBV research have helped lay the groundwork for the development and optimization of antiviral and immune-based therapeutic approaches that are now moving to clinical trials.
机译:审查抗病毒治疗慢性乙型肝炎感染的目的很少有治疗,因此HBV治愈策略的研究是优先事项。缺乏强大的细胞培养系统和小动物模型,药物开发和测试受到阻碍。本综述总结了HBV治愈研究的现有模型,并侧重于自2017年以来最近的发展。最近发现该领域在研究HBV的细胞培养和动物模型的发展中取得了进展。尽管早期细胞培养系统依赖于肝癌细胞系中转染HBV基因组,但表达HBV的进入受体的新型模型易受感染。改善原发性人肝细胞的培养条件,HBV的主要靶标,使筛查和验证了新的抗病毒。用部分人源化肝脏接枝的小鼠模型适用于测试病毒进入抑制剂或直接作用抗病毒,并且可以用人免疫细胞重构以分析免疫治疗。其他免疫合同模型包括用HBV基因组或用其天然肝炎病毒感染的HBV基因组或啄木枝转导的小鼠。 HBV研究的模型系统有助于为现在迁移到临床试验的抗病毒和免疫治疗方法的开发和优化奠定基础。

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