Cytochrome P-450-dependent biotransformation in Uje:WIST rats with chronic liver injury induced by thioacetamide.

Zeitschrift fur Versuchstierkunde Pub Date : 1989-01-01
H Kraul, T Zimmermann, C Pocha, J Truckenbrodt, A Hoffmann
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Abstract

In female Uje:WIST rats micronodular liver cirrhosis was produced by thioacetamide (TAA) given in the drinking water (0.3 g/l) from the 4th to 6th months of life. 14 d after TAA cessation it was examined, whether this animal model reflects the restricted cytochrome P-450-dependent biotransformation in severe stages of human liver cirrhosis by in vivo (caffeine and metamizol elimination) and in vitro methods (cytochrome P-450, 7-ethoxycoumarin and 7-ethoxyresorufin O-deethylation, ethylmorphine N-demethylation). The total biotransformation capacity was unchanged in TAA rats, partly even enhanced. Only several in vitro parameters reflect diminished cytochrome P-450-dependent biotransformation calculated per weight unit comparable to severe stages of human liver cirrhosis. Therefore, the chosen experimental conditions are suitable for conclusions concerning cytochrome P-450-dependent biotransformation in early rather than in severe stages of human liver cirrhosis.

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硫乙酰胺致慢性肝损伤Uje:WIST大鼠细胞色素p -450依赖性生物转化
雌性Uje:WIST大鼠从4 ~ 6个月开始在饮用水中添加硫乙酰胺(0.3 g/l),导致小结节性肝硬化。停用TAA后14 d,通过体内(咖啡因和甲胺唑消除)和体外(细胞色素P-450、7-乙氧基香豆素和7-乙氧基间苯甲酚o -去甲基化、乙基吗啡n -去甲基化)检测该动物模型是否反映了严重肝硬化阶段细胞色素P-450依赖性生物转化的限制性。TAA大鼠的总生物转化能力没有变化,甚至部分增强。只有几个体外参数反映细胞色素p -450依赖性生物转化的减少,每重量单位计算与人类肝硬化严重阶段相当。因此,所选择的实验条件适合于得出细胞色素p -450依赖性生物转化在人肝硬化早期而不是严重阶段的结论。
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