Rost K L, Brösicke H, Heinemeyer G, Roots I
Institute of Clinical Pharmacology, Klinikum Steglitz, Free University of Berlin, Germany.
Hepatology. 1994 Nov;20(5):1204-12.
Omeprazole induces hepatic cytochrome P-4501A2. In a previous study this effect was shown to be significant in vivo in 6 poor metabolizers, including 1 intermediate metabolizer, but not in 12 extensive metabolizers of S-mephenytoin after 7 days of treatment with 40 mg/day omeprazole. In this study, the specificity of the inducing potential of omeprazole was investigated in these volunteers. Furthermore, in eight of the extensive metabolizers the dose-dependence of cytochrome P-450 1A2 induction was evaluated. Cytochrome P-450 1A2 activity was monitored by means of the 13C-[N3-methyl]caffeine breath test and by means of plasma caffeine clearance before omeprazole treatment with 120 mg/day, on the seventh day of dosage and after a 7-day washout. Omeprazole plasma concentration was measured. Results were compared with those after 40 mg. gamma-Glutamyltransferase activity in serum, as well as urinary excretion of D-glucaric acid and 6 beta-hydroxycortisol, were measured on the same study days in all study groups (n = 26). In the eight extensive metabolizers the breath test indicated a dose-dependent increase of cytochrome P-450 1A2 activity of 8.5% +/- 15.0% (40 mg, mean +/- SD, NS) and 27.2% +/- 16.5% (120 mg, p = 0.002). Caffeine clearance was increased by 31.6% +/- 20.7% (p < 0.001) with the higher dose. None of the study groups exhibited a significant increase of gamma-glutamyltransferase activity or urinary excretion of D-glucaric acid or 6 beta-hydroxycortisol. This was in contrast to the phenobarbital-type induction observed after treatment with antiepileptic drugs. Induction by omeprazole seems to be restricted to cytochrome P-450 1A enzymes.(ABSTRACT TRUNCATED AT 250 WORDS)
奥美拉唑可诱导肝脏细胞色素P - 4501A2。在先前的一项研究中,在用40毫克/天的奥美拉唑治疗7天后,这种效应在6名代谢缓慢者(包括1名中间代谢者)体内显示出显著意义,但在12名S - 美芬妥因代谢正常者中未显示出显著意义。在本研究中,对这些志愿者中奥美拉唑诱导潜力的特异性进行了研究。此外,在8名代谢正常者中评估了细胞色素P - 450 1A2诱导的剂量依赖性。在使用120毫克/天的奥美拉唑治疗前、给药第7天以及7天洗脱期后,通过13C - [N3 - 甲基]咖啡因呼气试验和血浆咖啡因清除率来监测细胞色素P - 450 1A2活性。测量奥美拉唑血浆浓度。将结果与40毫克后的结果进行比较。在所有研究组(n = 26)的相同研究日测量血清中的γ - 谷氨酰转移酶活性以及D - 葡糖醛酸和6β - 羟基皮质醇的尿排泄量。在8名代谢正常者中,呼气试验表明细胞色素P - 450 1A2活性呈剂量依赖性增加,40毫克时为8.5%±15.0%(平均值±标准差,无显著性差异),120毫克时为27.2%±16.5%(p = 0.002)。较高剂量时咖啡因清除率增加了31.6%±20.7%(p < 0.001)。没有一个研究组的γ - 谷氨酰转移酶活性、D - 葡糖醛酸或6β - 羟基皮质醇的尿排泄量有显著增加。这与使用抗癫痫药物治疗后观察到的苯巴比妥型诱导情况相反。奥美拉唑的诱导作用似乎仅限于细胞色素P - 450 1A酶。(摘要截断于250字)
