奥美拉唑对细胞色素P450IA2活性的增强作用:通过13C-[N-3-甲基] -咖啡因呼气试验在S-美芬妥因慢代谢型和快代谢型个体中的证据。
Increase of cytochrome P450IA2 activity by omeprazole: evidence by the 13C-[N-3-methyl]-caffeine breath test in poor and extensive metabolizers of S-mephenytoin.
作者信息
Rost K L, Brösicke H, Brockmöller J, Scheffler M, Helge H, Roots I
机构信息
Institute of Clinical Pharmacology, Klinikum Steglitz, Free University of Berlin, Germany.
出版信息
Clin Pharmacol Ther. 1992 Aug;52(2):170-80. doi: 10.1038/clpt.1992.126.
Omeprazole has been shown to induce cytochrome P450IA1 and P450IA2 activity in vitro. To reflect cytochrome P450IA2 (CYP1A2) activity in vivo, the 13C-[N-3-methyl]-caffeine breath test was conducted in 18 volunteers: 12 extensive metabolizers, one intermediate metabolizer, and five poor metabolizers of S-mephenytoin. Breath tests were performed before treatment with an oral dose of 40 mg omeprazole, on the seventh day of treatment, and after a 7-day washout period. The mean percentage exhalation of the 13C test dose, as determined by 13CO2 in breath during 8 hours, was 23.0% +/- 8.0% (n = 18) before treatment. The largest increases in exhalation rate of 13CO2 were observed in the poor metabolizers and the intermediate metabolizers (range, 12.8% to 62.9%; median, 38.9%); median area under the plasma concentration-time curves (AUC) of omeprazole was four times higher than in the extensive metabolizers. The change after omeprazole treatment in extensive metabolizers ranged from -9.8% to +47.7% (median, 12.3%; n = 12) of pretreatment values. In both groups exhalation rates of 13CO2 returned to near pretreatment values within the 7-day washout period (24.2% +/- 7.8%; n = 17). Changes in the 13C-caffeine breath test correlated well with both the pretreatment value (R = -0.67, p = 0.003; n = 18) and the plasma AUC of omeprazole (R = 0.61, p = 0.007; n = 18). Therapeutic doses of omeprazole seem to induce CYP1A2 activity in poor metabolizers, whereas they exert minor inducing effects in extensive metabolizers of S-mephenytoin.
奥美拉唑已被证明在体外可诱导细胞色素P450IA1和P450IA2的活性。为反映体内细胞色素P450IA2(CYP1A2)的活性,对18名志愿者进行了13C-[N-3-甲基] -咖啡因呼气试验:其中12名S-美芬妥英的广泛代谢者、1名中间代谢者和5名慢代谢者。呼气试验在口服40mg奥美拉唑治疗前、治疗第7天以及7天的洗脱期后进行。治疗前,通过8小时内呼出气体中的13CO2测定,13C试验剂量的平均呼出百分比为23.0%±8.0%(n = 18)。慢代谢者和中间代谢者观察到13CO2呼出率的最大增幅(范围为12.8%至62.9%;中位数为38.9%);奥美拉唑的血浆浓度-时间曲线下面积(AUC)中位数比广泛代谢者高4倍。奥美拉唑治疗后,广泛代谢者的变化范围为治疗前值的-9.8%至+47.7%(中位数为12.3%;n = 12)。在两组中,13CO2呼出率在7天的洗脱期内均恢复至接近治疗前的值(24.2%±7.8%;n = 17)。13C-咖啡因呼气试验的变化与治疗前值(R = -0.67,p = 0.003;n = 18)和奥美拉唑的血浆AUC(R = 0.61,p = 0.007;n = 18)均密切相关。治疗剂量的奥美拉唑似乎可诱导慢代谢者的CYP1A2活性,而对S-美芬妥英的广泛代谢者则产生较小的诱导作用。
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