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Liver toxicity from norcocaine nitroxide, an N-oxidative metabolite of cocaine.

机译:硝可卡因的氮氧化物可卡因对肝脏的毒性。

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摘要

The oxidative metabolism of cocaine to norcocaine nitroxide has been postulated to be essential for cocaine hepatotoxicity. The hepatic effects of norcocaine nitroxide have never been evaluated in vivo, however. In this study mice were administered norcocaine nitroxide i.p., and hepatotoxicity was assessed using serum alanine aminotransferase activities and microscopic examination of liver tissue. Hepatotoxicity of norcocaine nitroxide was dose-related; significant injury was detectable at doses of 20 to 30 mg/kg i.p., and severe hepatocellular necrosis was observed at doses of 40 and 50 mg/kg. Elevated serum alanine aminotransferase activities peaked between 12 and 18 hr after norcocaine nitroxide treatment. Electron microscopy revealed the presence of pronounced changes in cell morphology as early as 30 min after the norcocaine nitroxide dose. Pretreatment of mice with phenobarbital had no effect on the magnitude of hepatic injury but shifted the intralobular site of necrosis from the midzonal to the periportal region. Pretreatment with diazinon, an esterase inhibitor, increased norcocaine nitroxide-induced liver damage, whereas each of the P450 inhibitors SKF 525A, cimetidine, troleandomycin, ketaconazole and chloramphenicol significantly diminished norcocaine nitroxide hepatotoxicity. The results indicate that norcocaine nitroxide is hepatotoxic and suggest the involvement of P450 enzymes.
机译:可卡因被氧化为可卡因氮氧化物的氧化代谢被认为对可卡因肝毒性至关重要。但是,从未在体内评估过氧化氮可卡因的肝脏作用。在该研究中,给小鼠腹膜内注射诺古卡因氮氧化物,并使用血清丙氨酸氨基转移酶活性和肝组织的显微镜检查来评估肝毒性。硝酸可卡因的肝毒性与剂量有关;腹膜内注射剂量为20至30 mg / kg时,可检测到明显的损伤,剂量为40和50 mg / kg时,可观察到严重的肝细胞坏死。硝酸可卡因治疗后12至18小时,血清丙氨酸氨基转移酶活性达到峰值。电子显微镜检查显示,在硝酸诺古卡因给药30分钟后,细胞形态就出现了明显的变化。苯巴比妥对小鼠的预处理对肝损伤的程度没有影响,但将小叶内坏死部位从中区转移到了门静脉区。用酯酶抑制剂二嗪农预处理可增加一氧化氮可卡因对肝脏的损害,而每种P450抑制剂SKF 525A,西咪替丁,曲雷曼霉素,ketaconazole和氯霉素均可显着降低一氧化氮可卡因的肝毒性。结果表明,诺卡卡因氮氧化物具有肝毒性,并提示P450酶参与其中。

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