塞来吉兰代谢和细胞色素P450酶:人肝微粒体的体外研究。

P Taavitsainen, M Anttila, L Nyman, H Karnani, J S Salonen, O Pelkonen
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引用次数: 24

摘要

虽然作为一种长期用于治疗的药物,但对其酶代谢的研究还不够充分。在体外实验中,我们研究了细胞色素P450 (CYP)催化selegiline氧化代谢为去甲基selegiline和1-甲基苯丙胺,以及selegiline、去甲基selegiline和1-甲基苯丙胺对人肝微粒体肝脏CYP酶的影响。去甲基selegiline和1-甲基苯丙胺生成的表观Km值平均为149 μ m和293 μ m,表观Vmax值为243 μ mol/min。/mg和1351 pmol/min。/毫克,分别。已知CYP1A2和CYP3A4的参比抑制剂Furafylline和酮康唑分别抑制去甲基selegiline的形成,Ki值分别为1.7和15微米。当Ki为18 μ m时,酮康唑对1-甲基苯丙胺的生成也有抑制作用。氟伏沙明是CYP1A2、CYP2C19和CYP3A4的抑制剂,在Ki值分别为9和25微米时抑制去甲基selegiline和1-甲基苯丙胺的形成。基于这些结果,我们认为CYP1A2和CYP3A4参与去甲基selegiline的形成,CYP3A4参与1-甲基苯丙胺的形成。在cyp5特异性模型活性研究中,selegiline和去甲基selegiline均抑制cyp2c19介导的s -甲苯基托因4'-羟基化,平均IC50值分别为21微米和26微米。测定selegiline的Ki值在7微米左右。Selegiline抑制cyp1a2介导的乙氧基间苯甲酚o -去甲基化,Ki值为76 μ m。selegiline、去甲基selegiline和1-甲基苯丙胺对其他cyp模型活性的抑制作用要低得多。在此基础上,我们发现selegiline和去甲基selegiline对CYP2C19具有较高的亲和力,但没有证据表明selegiline被CYP2C19代谢。
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Selegiline metabolism and cytochrome P450 enzymes: in vitro study in human liver microsomes.

Although being a drug therapeutically used for a long time, the enzymatic metabolism of selegiline has not been adequately studied. In the current work we have studied the cytochrome P450 (CYP)-catalyzed oxidative metabolism of selegiline to desmethylselegiline and 1-methamphetamine and the effects of selegiline, desmethylselegiline and 1-methamphetamine on hepatic CYP enzymes in human liver microsomes in vitro. The apparent Km values for desmethylselegiline and 1-methamphetamine formation were on an average 149 microM and 293 microM, and the apparent Vmax values, 243 pmol/min./mg and 1351 pmol/min./mg, respectively. Furafylline and ketoconazole, the known reference inhibitors for CYP1A2 and CYP3A4, respectively, inhibited the formation of desmethylselegiline with Ki value of 1.7 microM and 15 microM. Ketoconazole inhibited also the formation of 1-methamphetamine with Ki of 18 microM. Fluvoxamine, an inhibitor of CYP1A2, CYP2C19 and CYP3A4, inhibited the formation of desmethylselegiline and 1-methamphetamine with Ki values of 9 and 25 microM, respectively. On the basis of these results we suggest that CYP1A2 and CYP3A4 contribute to the formation of desmethylselegiline and that CYP3A4 participates in the formation of 1-methamphetamine. In studies with CYP-specific model activities, both selegiline and desmethylselegiline inhibited the CYP2C19-mediated S-mephenytoin 4'-hydroxylation with average IC50 values of 21 microM and 26 microM, respectively. The Ki for selegiline was determined to be around 7 microM. Selegiline inhibited CYP1A2-mediated ethoxyresorufin O-deethylation with a Ki value of 76 microM. Inhibitory potencies of selegiline, desmethylselegiline and 1-methamphetamine towards other CYP-model activities were much lower. On this basis, selegiline and desmethylselegiline were shown to have a relatively high affinity for CYP2C19, but no evidence about selegiline metabolism by CYP2C19 was obtained.

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