Inducible Nitric Oxide Synthase Expression in Liver Injury: Liver Protective Effects on Primary Rat Hepatocytes.

M. Kaibori, T. Okumura, Kenji Sato, M. Nishizawa, M. Kon
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引用次数: 22

Abstract

BACKGROUND/AIMS Following injury to the liver, liver cells, including Kupffer cells and hepatocytes express inducible nitric oxide synthase (iNOS), followed by the production of excess levels of nitric oxide (NO). NO produced by iNOS has been found to contribute to liver injury. Treatment of primary cultures of rat hepatocytes with the proinflammatory cytokine interleukin (IL)-1β stimulated iNOS expression and NO production. Experiments with this in vitro hepatocyte model of liver injury and with in vivo animal models of liver injury have demonstrated that drugs showing a liver-protective effect in vivo also inhibited the induction of iNOS expression and NO production both in vivo and in vitro. Thus, in this in vitro hepatocyte model, the prevention of iNOS expression and NO production are considered indicators of liver protection. RESULTS/CONCLUSION This review describes a simple in vitro liver injury model, consisting of IL-1β-stimulated cultured hepatocytes, and methods used to analyze the mechanisms of action of drugs that inhibit iNOS expression. This in vitro hepatocyte model may be used to assess the liver-protective effects of pharmaceutical agents, herbal medicines, and certain types of foods.
诱导型一氧化氮合酶在肝损伤中的表达:对原代大鼠肝细胞的保护作用。
背景/目的肝损伤后,肝细胞(包括库普弗细胞和肝细胞)表达诱导型一氧化氮合酶(iNOS),随后产生过量的一氧化氮(NO)。iNOS产生的NO已被发现有助于肝损伤。用促炎细胞因子白细胞介素(IL)-1β处理大鼠肝细胞原代培养物可刺激iNOS表达和NO生成。通过体外肝损伤肝细胞模型和体内肝损伤动物模型的实验表明,在体内具有保肝作用的药物在体内和体外均能抑制诱导iNOS表达和NO生成。因此,在体外肝细胞模型中,抑制iNOS的表达和NO的产生被认为是保护肝脏的指标。结果/结论本文介绍了一种由il -1β刺激的培养肝细胞组成的简单体外肝损伤模型,并分析了抑制iNOS表达的药物的作用机制。这种体外肝细胞模型可用于评估药物制剂、草药和某些类型的食物对肝脏的保护作用。
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