首页> 外文期刊>Toxicologic pathology >Human hepatocytes can repopulate mouse liver: histopathology of the liver in human hepatocyte-transplanted chimeric mice and toxicologic responses to acetaminophen.
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Human hepatocytes can repopulate mouse liver: histopathology of the liver in human hepatocyte-transplanted chimeric mice and toxicologic responses to acetaminophen.

机译:人肝细胞可以重新填充小鼠肝脏:人肝细胞移植嵌合小鼠的肝脏组织病理学和对乙酰氨基酚的毒理学反应。

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摘要

A human hepatocyte-transplanted chimeric mouse has been established by transplantation of human hepatocytes to urokinase-type plasminogen activator transgenic/severe combined immunodeficiency (uPA(+/+)/SCID) mice. These chimeric mice have various amounts of human hepatocytes that proliferate extensively and progressively replace mouse hepatocytes. In the chimeric liver, hepatic cords and sinusoid-like structures were observed. The human hepatocytes expressed human albumin, human cytochrome P450 enzymes, and human transporter proteins. Furthermore, electron microscopic analysis demonstrated bile canaliculi associated with human hepatocytes in the chimeric mouse livers. These results indicate that the chimeric mouse livers contain functionally intact and differentiated human hepatocytes. Additionally, the toxicologic response of hepatocytes to acetaminophen (APAP) administration was compared in normal and chimeric mouse livers. Following 1,400 mg/kg APAP, mild hepatocellular degeneration was observed in the human hepatocyte areas in the chimeric mice, compared with severe centrilobular hepatocellular necrosis in the ICR mouse livers. In conclusion, these chimeric livers contain functionally differentiated human hepatocytes, and are less susceptible to APAP toxicity, compared to ICR mice.
机译:通过将人类肝细胞移植到尿激酶型纤溶酶原激活物转基因/严重联合免疫缺陷(uPA(+ / +)/ SCID)小鼠中,已经建立了人类肝细胞移植嵌合小鼠。这些嵌合小鼠具有大量增殖并逐渐替代小鼠肝细胞的人类肝细胞。在嵌合肝中,观察到肝索和正弦样结构。人肝细胞表达人白蛋白,人细胞色素P450酶和人转运蛋白。此外,电子显微镜分析显示嵌合小鼠肝脏中与人肝细胞相关的胆小管。这些结果表明,嵌合小鼠肝脏含有功能完整和分化的人肝细胞。此外,比较了正常和嵌合小鼠肝脏中肝细胞对乙酰氨基酚(APAP)的毒理反应。在1,400 mg / kg APAP之后,与在ICR小鼠肝脏中严重的小叶肝细胞坏死相比,在嵌合小鼠的人肝细胞区域观察到轻度肝细胞变性。总之,与ICR小鼠相比,这些嵌合肝含有功能分化的人肝细胞,对APAP毒性的敏感性较低。

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