Kuhlmann J, Dohrmann M, Marcin S
Clin Pharmacol Ther. 1986 Mar;39(3):288-94. doi: 10.1038/clpt.1986.41.
Quinidine has been reported to increase digoxin plasma concentrations, which increases the risk of digoxin overdose. The effect of quinidine on digitoxin pharmacokinetics is still controversial because most studies were not performed with subjects achieving definite steady-state conditions. To determine whether quinidine affects digitoxin kinetics and cardiac efficacy, we measured glycoside plasma concentrations and renal excretion as well as ECG parameters and systolic time intervals before and during quinidine dosing in eight healthy subjects at steady state. Mean (+/- SD) digitoxin plasma concentrations and renal excretion increased from 13.6 +/- 2.2 ng/ml and 16.1 +/- 5.8 micrograms/24 hours before dosing to 19.7 +/- 3.1 ng/ml and 23.4 +/- 4.9 micrograms/24 hours, respectively, during quinidine dosing for 32 days. While renal digitoxin clearance was not noticeably changed by quinidine, total digitoxin clearance and extrarenal digitoxin clearance decreased by an average of 32% and 40.5%, respectively. The elimination t1/2 was prolonged from 150.3 +/- 20.6 to 202.6 +/- 37.5 hours. The increased digitoxin plasma level is pharmacodynamically active. We conclude that there is a clinically important interaction between digitoxin and quinidine, but it is to a lesser extent and is caused by different mechanism, in part, than the interaction between digoxin and quinidine.
据报道,奎尼丁可提高地高辛的血浆浓度,从而增加地高辛过量的风险。奎尼丁对洋地黄毒苷药代动力学的影响仍存在争议,因为大多数研究并非在达到明确稳态条件的受试者中进行。为了确定奎尼丁是否影响洋地黄毒苷的动力学和心脏效应,我们在8名处于稳态的健康受试者中,测量了奎尼丁给药前和给药期间的糖苷血浆浓度、肾排泄以及心电图参数和收缩期时间间期。在32天的奎尼丁给药期间,洋地黄毒苷的平均(±标准差)血浆浓度和肾排泄分别从给药前的13.6±2.2 ng/ml和16.1±5.8μg/24小时增加到19.7±3.1 ng/ml和23.4±4.9μg/24小时。虽然奎尼丁对洋地黄毒苷的肾清除率没有明显改变,但洋地黄毒苷的总清除率和肾外清除率分别平均下降了32%和40.5%。消除半衰期从150.3±20.6小时延长至202.6±37.5小时。洋地黄毒苷血浆水平的升高具有药效学活性。我们得出结论,洋地黄毒苷和奎尼丁之间存在具有临床重要性的相互作用,但与地高辛和奎尼丁之间的相互作用相比,其程度较小且部分是由不同机制引起的。
