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混合功能氧化酶诱导剂和抑制剂对喷他卡因代谢物胆汁排泄的影响。

Effects of inducers and inhibitors of mixed-function oxidases on the biliary excretion of pentacaine metabolites.

作者信息

Kukan M, Bezek S, Scasnár V, Durisová M, Trnovec T

机构信息

Institute of Experimental Pharmacology, Slovak Academy of Sciences, Bratislava.

出版信息

Biopharm Drug Dispos. 1990 Jul;11(5):395-401. doi: 10.1002/bdd.2510110504.

Abstract

The biliary excretion of 3H-pentacaine and its metabolites was studied in rats pretreated with an inducer or inhibitor of mixed-function oxidases. Over one-fourth (25.8 per cent) of a 2 mg kg-1 intraportal dose of 3H-pentacaine was excreted in bile in urethaneanaesthetized control rats within 3 h. The radioactivity appeared in the form of the parent drug, basic metabolites, and metabolite conjugates, 3.1, 86.5, and 10.4 per cent of the total radioactivity excreted, respectively. Pretreatment of rats with phenobarbital enhanced only slightly the biliary excretion of basic metabolites, and pretreatment with 3-methylcholanthrene had no effect. Phenobarbital also increased the initial rate of excretion of conjugates, but this effect was not sustained. 3-Methylcholanthrene had a tendency to impair excretion of conjugates by bile. Pretreatment of rats with SKF 525-A decreased the biliary excretion of both basic metabolites and conjugates while cimetidine did not alter significantly the biliary excretion of pentacaine metabolites. These results suggest that the canalicular transport of metabolites may be the most important factor in controlling pentacaine metabolite excretion in bile.

摘要

在经混合功能氧化酶诱导剂或抑制剂预处理的大鼠中,研究了3H-喷他卡因及其代谢产物的胆汁排泄情况。在氨基甲酸乙酯麻醉的对照大鼠中,门静脉内注射2mg/kg剂量的3H-喷他卡因后,超过四分之一(25.8%)的药物在3小时内随胆汁排出。放射性以母体药物、碱性代谢产物和代谢产物结合物的形式出现,分别占总排泄放射性的3.1%、86.5%和10.4%。用苯巴比妥预处理大鼠仅轻微增强了碱性代谢产物的胆汁排泄,而用3-甲基胆蒽预处理则无影响。苯巴比妥还增加了结合物的初始排泄速率,但这种作用未持续。3-甲基胆蒽有损害胆汁结合物排泄的趋势。用SKF 525-A预处理大鼠可降低碱性代谢产物和结合物的胆汁排泄,而西咪替丁对喷他卡因代谢产物的胆汁排泄无显著影响。这些结果表明,代谢产物的小管转运可能是控制喷他卡因代谢产物胆汁排泄的最重要因素。

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