Johne A, Brockmöller J, Bauer S, Maurer A, Langheinrich M, Roots I
Institute of Clinical Pharmacology, University Medical Center Charité, Humboldt University, Berlin, Germany.
Clin Pharmacol Ther. 1999 Oct;66(4):338-45. doi: 10.1053/cp.1999.v66.a101944.
Extracts of St John's wort (Hypericum perforatum) are widely used in the treatment of depression, often as an over-the-counter drug. In contrast to its frequent use, knowledge about the pharmacokinetics of ingredients and drug interactions of St John's wort is poor. We studied the interaction between hypericum extract LI160 and digoxin.
The pharmacokinetics of digoxin were investigated in a single-blind, placebo-controlled parallel study. After the achievement of steady state for digoxin on day 5, healthy volunteers received digoxin (0.25 mg/d) either with placebo (n = 12) or with 900 mg/d LI160 (n = 13) for another 10 days. Digoxin concentration profiles on day 5 were compared with day 6 (single-dose interaction) and day 15 (tenth day of co-medication).
There was a highly significant combined-day-and-group effect for digoxin area under the plasma concentration-time curve [AUC(0-24); P = .0001], peak concentration in plasma (Cmax; P = .0001), and plasma drug concentration at the end of a dosing interval (P = .0003) by two-way ANOVA. No statistically significant change was observed after the first dose of hypericum extract [AUC(0-24) at day 6 of 18.1+/-2.9 microg x h/L and 17.7+/-3.0 microg x h/L, mean +/- SD for placebo and hypericum group, respectively]. However, 10 days of treatment with hypericum extract resulted in a decrease of digoxin AUC(0-24) by 25% (day 15, 17.2+/-4.0 microg x h/L and 12.9+/-2.3 microg x h/L; P = .0035). Furthermore, comparison with the parallel placebo group after multiple dosing showed a reduction in trough concentrations and Cmax of 33% (P = .0023) and 26% (P = .0095), respectively. The effect became increasingly pronounced until the tenth day of co-medication.
As with grapefruit juice, a food product, physicians should also be aware of potential drug-herb interactions. The interaction of St John's wort extract with digoxin kinetics was time dependent. The mechanism involved may be induction of the P-glycoprotein drug transporter.
圣约翰草提取物(贯叶连翘)被广泛用于治疗抑郁症,常作为非处方药。尽管其使用频繁,但关于圣约翰草成分的药代动力学及药物相互作用的了解却很少。我们研究了金丝桃提取物LI160与地高辛之间的相互作用。
在一项单盲、安慰剂对照的平行研究中对地高辛的药代动力学进行了研究。在第5天达到地高辛稳态后,健康志愿者接受地高辛(0.25mg/d),一组服用安慰剂(n = 12),另一组服用900mg/d的LI160(n = 13),持续10天。比较第5天、第6天(单剂量相互作用)和第15天(联合用药第10天)的地高辛浓度曲线。
通过双向方差分析,地高辛血浆浓度-时间曲线下面积[AUC(0 - 24)]、血浆峰浓度(Cmax)和给药间隔末期的血浆药物浓度存在高度显著的联合日和组效应(P = .0001、P = .0001、P = .0003)。服用第一剂金丝桃提取物后未观察到统计学上的显著变化[安慰剂组和金丝桃组第6天的AUC(0 - 24)分别为18.1±2.9μg·h/L和17.7±3.0μg·h/L,均值±标准差]。然而,服用金丝桃提取物10天后,地高辛的AUC(0 - 24)降低了25%(第15天,分别为17.2±4.0μg·h/L和12.9±2.3μg·h/L;P = .0035)。此外,多次给药后与平行安慰剂组比较,谷浓度和Cmax分别降低了33%(P = .0023)和26%(P = .0095)。这种效应在联合用药第10天之前愈发明显。
与食品葡萄柚汁一样,医生也应意识到潜在的药物与草药相互作用。圣约翰草提取物与地高辛动力学的相互作用具有时间依赖性。其涉及的机制可能是P - 糖蛋白药物转运体的诱导。
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