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Generation of a humanized mouse model with both human immune system and liver cells to model hepatitis C virus infection and liver immunopathogenesis

机译:与人类免疫系统和肝细胞模型丙型肝炎病毒感染和免疫学肝的人源化小鼠模型的生成

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摘要

Establishing a small animal model that accurately recapitulates hepatotropic pathogens, including hepatitis C virus (HCV) infection and immunopathogenesis, is essential for the study of hepatitis virus–induced liver disease and for therapeutics development. This protocol describes our recently developed humanized mouse model for studying HCV and other hepatotropic infections, human immune response and hepatitis and liver fibrosis. The first 5-h stage is the isolation of human liver progenitor and hematopoietic stem cells from fetal liver. Next, AFC8 immunodeficient mice are transplanted with the isolated progenitor/stem cells. This generally takes 2 h. The transplanted mice are then treated for a month with the mouse liver apoptosis–inducing AFC8 dimerizer and left for an additional 2-month period to permit human liver and immune cell growth as well as system reconstitution and development before inoculation with HCV clinical isolates. HCV infection, human immune response and liver disease are observed with high incidence from approximately 2 months after inoculation.
机译:建立一个能准确概括包括丙型肝炎病毒(HCV)感染和免疫发病机制在内的肝病性病原体的小型动物模型,对于研究由肝炎病毒引起的肝病和治疗方法的发展至关重要。该协议描述了我们最近开发的人源化小鼠模型,用于研究HCV和其他肝硬化感染,人类免疫反应以及肝炎和肝纤维化。第一个5小时的阶段是从胎儿肝脏中分离人类肝脏祖细胞和造血干细胞。接下来,将AFC8免疫缺陷小鼠移植到分离的祖细胞/干细胞中。这通常需要2个小时。然后将移植的小鼠用诱导小鼠肝细胞凋亡的AFC8二聚体处理一个月,再放置2个月,以使人肝和免疫细胞生长以及系统重组和发育,然后再接种HCV临床分离株。接种后约两个月,HCV感染,人类免疫反应和肝病的发病率很高。

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