Petsalo Aleksanteri, Turpeinen Miia, Pelkonen Olavi, Tolonen Ari
Novamass Ltd, Medipolis Center, Kiviharjuntie 11, 90220 Oulu, Finland.
J Chromatogr A. 2008 Dec 26;1215(1-2):107-15. doi: 10.1016/j.chroma.2008.10.122. Epub 2008 Nov 7.
An LC/MS/MS method was developed for the analysis of twelve cytochrome P450 (CYP)-specific probe metabolites and their nine parent drugs from human urine. CYP-specific metabolites of melatonin (CYP1A2), nicotine (CYP2A6), bupropion (CYP2B6), repaglinide (CYP2C8), losartan (CYP2C9), omeprazole (CYP2C19 and CYP3A4), dextromethorphan (CYP2D6), chlorzoxazone (CYP2E1) and midazolam (CYP3A4) were all analyzed using the same LC/MS/MS method with a single analytical run, either after a one-at-a-time dose or cocktail-type dosing of the parent drugs. Ultra performance liquid chromatography (UPLC) with a 1.7 microm particle size column was utilized, providing 1.5-3-fold increase in sensitivity, decrease of analysis time to one third and clearly better chromatographic peak shapes when comparing it with the method using traditional high performance liquid chromatography for the same metabolites. In addition, the method was applied for the analysis of the metabolites from human urine samples collected at multiple time points after single and N-in-one dosing of each of the drugs, showing that the use of both the analytical method and these probe metabolites as CYP-specific markers is feasible in in vivo drug-drug interaction or phenotyping studies.
建立了一种液相色谱/串联质谱(LC/MS/MS)方法,用于分析人尿液中12种细胞色素P450(CYP)特异性探针代谢物及其9种母体药物。褪黑素(CYP1A2)、尼古丁(CYP2A6)、安非他酮(CYP2B6)、瑞格列奈(CYP2C8)、氯沙坦(CYP2C9)、奥美拉唑(CYP2C19和CYP3A4)、右美沙芬(CYP2D6)、氯唑沙宗(CYP2E1)和咪达唑仑(CYP3A4)的CYP特异性代谢物均采用相同的LC/MS/MS方法在单次分析运行中进行分析,母体药物采用单次给药或鸡尾酒式给药。使用了粒径为1.7微米的超高效液相色谱(UPLC)柱,与使用传统高效液相色谱分析相同代谢物的方法相比,灵敏度提高了1.5至3倍,分析时间缩短至三分之一,色谱峰形明显更好。此外,该方法还应用于分析每种药物单次给药和N合一给药后在多个时间点采集的人尿液样本中的代谢物,结果表明,将该分析方法和这些探针代谢物用作CYP特异性标记物在体内药物相互作用或表型研究中是可行的。
