单次应用透皮给药系统后毒扁豆碱在人体的药代动力学。
Pharmacokinetics of physostigmine in man following a single application of a transdermal system.
作者信息
Walter K, Müller M, Barkworth M F, Nieciecki A V, Stanislaus F
机构信息
Klinge Pharma GmbH, Munich, Germany.
出版信息
Br J Clin Pharmacol. 1995 Jan;39(1):59-63. doi: 10.1111/j.1365-2125.1995.tb04410.x.
Abstract
- The pharmacokinetics of physostigmine were investigated in a three-way cross-over design in six healthy, male volunteers comparing a physostigmine transdermal system (PTS), an oral solution and an i.v. infusion. 2. A single application of the patch over 24 h produced detectable plasma drug concentrations after a mean lag-time of 4 h. Thereafter, the drug was absorbed continuously from the PTS and putative therapeutic plasma concentrations were measured over approximately 18 h. 3. A mean absolute bioavailability of 36% was determined for the transdermal system and 3% for the oral solution. In comparison with the oral solution, interindividual variability of pharmacokinetics was less with the PTS. 4. The mean amount of physostigmine released from the transdermal system after 24 h was 5.7 mg. Because of extensive metabolism, only 2.2 mg of physostigmine were detected systemically. 5. After removing the PTS, the mean apparent half-life of elimination was 4.9 h, compared with 0.5 h for the i.v. infusion. This indicates continued drug absorption from a skin depot. 6. Physostigmine was well tolerated by the volunteers. With the PTS, a mild erythema was observed at the area of application, disappearing within a few hours.
摘要
- 在一项三交叉设计中,对6名健康男性志愿者研究了毒扁豆碱的药代动力学,比较了毒扁豆碱透皮系统(PTS)、口服溶液和静脉输注。2. 在24小时内单次应用贴片后,平均滞后4小时可检测到血浆药物浓度。此后,药物从PTS持续吸收,并在约18小时内测量推定的治疗性血浆浓度。3. 透皮系统的平均绝对生物利用度为36%,口服溶液为3%。与口服溶液相比,PTS的药代动力学个体间变异性较小。4. 24小时后,透皮系统释放的毒扁豆碱平均量为5.7毫克。由于广泛代谢,全身仅检测到2.2毫克毒扁豆碱。5. 去除PTS后,平均表观消除半衰期为4.9小时,静脉输注为0.5小时。这表明药物从皮肤贮库持续吸收。6. 志愿者对毒扁豆碱耐受性良好。使用PTS时,在应用部位观察到轻度红斑,数小时内消失。
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