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美沙酮对人细胞色素P450 2D6(CYP2D6)的抑制作用。

Inhibition of human cytochrome P450 2D6 (CYP2D6) by methadone.

作者信息

Wu D, Otton S V, Sproule B A, Busto U, Inaba T, Kalow W, Sellers E M

机构信息

Clinical Research and Treatment Institute, Addiction Research Foundation, Toronto, Ontario, Canada.

出版信息

Br J Clin Pharmacol. 1993 Jan;35(1):30-4. doi: 10.1111/j.1365-2125.1993.tb05666.x.

Abstract
  1. In microsomes prepared from three human livers, methadone competitively inhibited the O-demethylation of dextromethorphan, a marker substrate for CYP2D6. The apparent Ki value of methadone ranged from 2.5 to 5 microM. 2. Two hundred and fifty-two (252) white Caucasians, including 210 unrelated healthy volunteers and 42 opiate abusers undergoing treatment with methadone were phenotyped using dextromethorphan as the marker drug. Although the frequency of poor metabolizers was similar in both groups, the extensive metabolizers among the opiate abusers tended to have higher O-demethylation metabolic ratios and to excrete less of the dose as dextromethorphan metabolites than control extensive metabolizer subjects. These data suggest inhibition of CYP2D6 by methadone in vivo as well. 3. Because methadone is widely used in the treatment of opiate abuse, inhibition of CYP2D6 activity in these patients might contribute to exaggerated response or unexpected toxicity from drugs that are substrates of this enzyme.
摘要
  1. 在从三个人类肝脏制备的微粒体中,美沙酮竞争性抑制右美沙芬的O-去甲基化,右美沙芬是CYP2D6的一种标记底物。美沙酮的表观Ki值范围为2.5至5微摩尔。2. 252名白种人,包括210名无亲缘关系的健康志愿者和42名接受美沙酮治疗的阿片类药物滥用者,使用右美沙芬作为标记药物进行了表型分析。虽然两组中代谢不良者的频率相似,但阿片类药物滥用者中的广泛代谢者往往具有更高的O-去甲基化代谢率,并且与对照广泛代谢者相比,作为右美沙芬代谢物排泄的剂量更少。这些数据也表明美沙酮在体内抑制CYP2D6。3. 由于美沙酮广泛用于治疗阿片类药物滥用,这些患者中CYP2D6活性的抑制可能导致该酶底物药物的反应过度或意外毒性。

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