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原代纯培养和混合单层培养的大鼠成年肝细胞。药物代谢中混合功能氧化酶和结合途径维持情况的比较。

Rat adult hepatocytes in primary pure and mixed monolayer culture. Comparison of the maintenance of mixed function oxidase and conjugation pathways of drug metabolism.

作者信息

Niemann C, Gauthier J C, Richert L, Ivanov M A, Melcion C, Cordier A

机构信息

Institut de Recherche sur la sécurité de Médicament, Centre de Recherches de Vitry-Alfortville, Vitry sur Seine, France.

出版信息

Biochem Pharmacol. 1991 Jul 5;42(2):373-9. doi: 10.1016/0006-2952(91)90725-k.

Abstract

The stabilities of several drug oxidation and conjugation pathways in adult rat hepatocytes were investigated in two systems: a primary pure culture lasting 3 days and a primary mixed culture (hepatocytes co-cultured with epithelial cells) lasting 10 days. The cytochrome P450 content in hepatocytes drastically declined within 48 hr in both culture systems. Cytochrome P450-dependent mixed function oxidase was measured by the O-dealkylation of ethoxyresorufin (EROD) and of pentoxyresorufin (PROD). UPD-glucuronosyl transferase (UDP-GT) activity was measured using 1-naphthol and morphine as substrates. In both culture systems, the activities of enzymes belonging to the 3-methylcholanthrene-inducible family, namely EROD and 1-naphthol UDP-GT, were much better maintained than those of PROD and morphine UDP-GT, which belong to the phenobarbitone-inducible family: in pure cultures, EROD and 1-naphthol UDP-GT activities declined to 60% of initial values within 3 days; in mixed cultures, EROD activity was stable throughout the 10 day culture period, whereas that of 1-naphthol UDP-GT was stable until day 4 but had declined to 70% of the initial value by day 8. In contrast, PROD and morphine UDP-GT activities declined to approx. 30% of the initial values within 2 days in both culture systems, and had dropped to approx. 10% of the initial value within 8 days in mixed culture. Reduced glutathione (GSH) levels fluctuated, but remained high throughout culture. GSH conjugation declined to 40% of initial values within 3 days in pure culture, whereas it remained relatively constant in mixed culture. Comparison of these two culture systems therefore showed that although the inclusion of epithelial cells did prolong hepatocyte viability, there was a change in relative enzyme activities in both systems, suggesting a shift towards a more de-differentiated drug metabolism pattern.

摘要

在两个系统中研究了成年大鼠肝细胞中几种药物氧化和结合途径的稳定性

一种是持续3天的原代纯培养,另一种是持续10天的原代混合培养(肝细胞与上皮细胞共培养)。在两种培养系统中,肝细胞中的细胞色素P450含量在48小时内急剧下降。通过乙氧基试卤灵(EROD)和戊氧基试卤灵(PROD)的O-脱烷基化来测定细胞色素P450依赖性混合功能氧化酶。使用1-萘酚和吗啡作为底物来测定尿苷二磷酸葡萄糖醛酸基转移酶(UDP-GT)活性。在两种培养系统中,属于3-甲基胆蒽诱导家族的酶,即EROD和1-萘酚UDP-GT的活性,比属于苯巴比妥诱导家族的PROD和吗啡UDP-GT的活性保持得更好:在纯培养中,EROD和1-萘酚UDP-GT活性在3天内降至初始值的60%;在混合培养中,EROD活性在整个10天培养期内稳定,而1-萘酚UDP-GT的活性直到第4天稳定,但到第8天已降至初始值的70%。相比之下,在两种培养系统中,PROD和吗啡UDP-GT活性在2天内降至初始值的约30%,在混合培养中8天内已降至初始值的约10%。还原型谷胱甘肽(GSH)水平波动,但在整个培养过程中保持较高。在纯培养中,GSH结合在3天内降至初始值的40%,而在混合培养中保持相对恒定。因此,这两种培养系统的比较表明,虽然上皮细胞的加入确实延长了肝细胞的活力,但两种系统中相对酶活性都发生了变化,这表明向更去分化的药物代谢模式转变。

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