人源化肝脏 NSG-PiZ 小鼠支持慢性乙型肝炎病毒感染和抗病毒治疗的研究。
Liver-Humanized NSG-PiZ Mice Support the Study of Chronic Hepatitis B Virus Infection and Antiviral Therapies.
机构信息
Vaccine and Infectious Disease Division, Fred Hutchinson Cancer Center, Seattle, Washington, USA.
Department of Laboratory Medicine and Pathology, University of Washington, Seattle, Washington, USA.
出版信息
Microbiol Spectr. 2023 Jun 15;11(3):e0517622. doi: 10.1128/spectrum.05176-22. Epub 2023 May 18.
Hepatitis B virus (HBV) is a pathogen of major public health importance that is largely incurable once a chronic infection is established. Only humans and great apes are fully permissive to HBV infection, and this species restriction has impacted HBV research by limiting the utility of small animal models. To combat HBV species restrictions and enable more studies, liver-humanized mouse models have been developed that are permissive to HBV infection and replication. Unfortunately, these models can be difficult to establish and are expensive commercially, which has limited their academic use. As an alternative mouse model to study HBV, we evaluated liver-humanized NSG-PiZ mice and showed that they are fully permissive to HBV. HBV selectively replicates in human hepatocytes within chimeric livers, and HBV-positive (HBV) mice secrete infectious virions and hepatitis B surface antigen (HBsAg) into blood while also harboring covalently closed circular DNA (cccDNA). HBV mice develop chronic infections lasting at least 169 days, which should enable the study of new curative therapies targeting chronic HBV, and respond to entecavir therapy. Furthermore, HBV human hepatocytes in NSG-PiZ mice can be transduced by AAV3b and AAV.LK03 vectors, which should enable the study of gene therapies that target HBV. In summary, our data demonstrate that liver-humanized NSG-PiZ mice can be used as a robust and cost-effective alternative to existing chronic hepatitis B (CHB) models and may enable more academic research labs to study HBV disease pathogenesis and antiviral therapy. Liver-humanized mouse models have become the gold standard for the study of hepatitis B virus (HBV), yet their complexity and cost have prohibited widespread use of existing models in research. Here, we show that the NSG-PiZ liver-humanized mouse model, which is relatively inexpensive and simple to establish, can support chronic HBV infection. Infected mice are fully permissive to hepatitis B, supporting both active replication and spread, and can be used to study novel antiviral therapies. This model is a viable and cost-effective alternative to other liver-humanized mouse models that are used to study HBV.
乙型肝炎病毒 (HBV) 是一种具有重要公共卫生意义的病原体,一旦发生慢性感染,基本上是无法治愈的。只有人类和大型猿类才完全允许 HBV 感染,这种物种限制通过限制小动物模型的应用,影响了 HBV 研究。为了克服 HBV 的物种限制并促进更多的研究,已经开发了允许 HBV 感染和复制的肝人源化小鼠模型。不幸的是,这些模型可能难以建立,并且商业上价格昂贵,这限制了它们在学术上的使用。作为研究 HBV 的替代小鼠模型,我们评估了肝人源化 NSG-PiZ 小鼠,并表明它们完全允许 HBV 感染。HBV 在嵌合肝脏中的人肝细胞中选择性复制,HBV 阳性 (HBV) 小鼠将传染性病毒颗粒和乙型肝炎表面抗原 (HBsAg) 分泌到血液中,同时还携带共价闭合环状 DNA (cccDNA)。HBV 小鼠发生持续至少 169 天的慢性感染,这应该能够研究针对慢性 HBV 的新治疗方法,并对恩替卡韦治疗产生反应。此外,NSG-PiZ 小鼠中的 HBV 人肝细胞可以被 AAV3b 和 AAV.LK03 载体转导,这应该能够研究针对 HBV 的基因治疗方法。总之,我们的数据表明,肝人源化 NSG-PiZ 小鼠可以作为现有慢性乙型肝炎 (CHB) 模型的强大且具有成本效益的替代方案,并且可能使更多的学术研究实验室能够研究 HBV 疾病发病机制和抗病毒治疗。 肝人源化小鼠模型已成为乙型肝炎病毒 (HBV) 研究的金标准,但它们的复杂性和成本限制了现有模型在研究中的广泛应用。在这里,我们表明,相对便宜且易于建立的 NSG-PiZ 肝人源化小鼠模型可以支持慢性 HBV 感染。感染的小鼠对乙型肝炎完全允许,支持病毒的活跃复制和传播,并可用于研究新型抗病毒疗法。该模型是用于研究 HBV 的其他肝人源化小鼠模型的可行且具有成本效益的替代方案。
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