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机构地区:[1]白求恩国际和平医院临床药理室,河北石家庄050082
出 处:《药学学报》2004年第8期581-585,共5页Acta Pharmaceutica Sinica
摘 要:目的 研究反式曲马朵 (transT)对映体代谢 ,反式氧去甲基曲马朵 (M1)对映体生成及其与葡糖醛酸结合的性别差异。方法 以transT或M1为底物分别与大鼠肝微粒体孵育 ,高效毛细管电泳法测定孵育液中transT和M1对映体。结果 与 (+) 对映体相比 ,(- ) transT优先代谢 ,(- ) M1优先生成。在雌性大鼠肝微粒体中 (- ) M1优先与葡糖醛酸结合 ;M1两对映体生成及其与葡糖醛酸结合的CLint比值偏离 1的程度较大。在雄性大鼠肝微粒体中 (+) M1优先与葡糖醛酸结合。结论 TransT代谢 ,M1生成及其与葡糖醛酸结合均具立体选择性和性别差异 ;Aim To investigate the gender-related differences in the metabolism of trans tramadol (trans T) enantiomers and the glucuronidation of trans O-demethyltramadol (M1) enantiomers. Methods In vitro, trans T or M1 were separately incubated with liver microsomes of male or female rats. The concentrations of the enantiomers of trans T and M1 were determined by an HPCE method.Results Compared with (+)-enantiomers, (-)-trans T was preferentially metabolized, and (-)-M1 was produced faster in rat liver microsomes. (+)-M1 and (-)-M1 were preferentially glucuronidated in the liver microsomes of male and female rats, respectively. Compared with those in male rat liver microsomes, the enantiomeric ratios of CL int for M1 formation and M1 glucuronidation were more deviated from 1 in female rat liver microsomes. Conclusion In vitro, trans T metabolism, M1 formation and M1 glucuronidation were found to be stereoselective in rat liver microsomes. There were gender-related differences in the stereoselectivity in M1 formation and M1 glucuronidation, with a larger extent in female rat liver microsomes.
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