对健康受试者进行吗啡的经皮给药。
Transdermal administration of morphine to healthy subjects.
作者信息
Westerling D, Höglund P, Lundin S, Svedman P
机构信息
Department of Anaesthesiology, University of Lund, Sweden.
出版信息
Br J Clin Pharmacol. 1994 Jun;37(6):571-6. doi: 10.1111/j.1365-2125.1994.tb04306.x.
Abstract
- Twelve healthy subjects received 10 mg morphine HCl delivered transdermally from an occlusive reservoir applied to a small area of skin, painlessly de-epithelialised by vacuum suction. On a separate occasion, 10 mg morphine HCl was given as an i.v. infusion over 20 min. 2. Venous blood samples were collected serially for 72 h and assayed for morphine, morphine-3-glucuronide (M3G) and morphine-6-glucuronide (M6G) by h.p.l.c. Pupil size, salivation, and central nervous effects (nausea, fatigue, headache, feeling of heaviness and dysphoria/euphoria) were also measured. 3. After transdermal application morphine was absorbed by a first-order process to produce relatively constant plasma drug concentrations over 11 h. The absolute bioavailability of transdermal morphine was 75% (65-85%; 95% CI). The plasma concentrations of both M6G and M3G were lower after transdermal administration than after i.v. infusion, and a considerable delay (of up to 1 h) was observed before the metabolites were detectable. AUC ratios for M3G and M6G relative to morphine were similar after both modes of administration. 4. Non-analgesic effects were less pronounced at the lower plasma drug and metabolite concentrations observed after transdermal delivery than after the i.v. infusion of morphine. 5. Transdermal administration of morphine warrants investigation as an alternative route of morphine delivery.
摘要
- 12名健康受试者接受了经皮给予的10毫克盐酸吗啡,药物由一个封闭储库提供,该储库贴于一小片经真空抽吸无痛去上皮的皮肤上。在另一个时间点,以静脉输注的方式在20分钟内给予10毫克盐酸吗啡。2. 连续72小时采集静脉血样,采用高效液相色谱法测定其中的吗啡、吗啡-3-葡萄糖醛酸苷(M3G)和吗啡-6-葡萄糖醛酸苷(M6G)。还测量了瞳孔大小、唾液分泌以及中枢神经效应(恶心、疲劳、头痛、沉重感和烦躁/欣快感)。3. 经皮给药后,吗啡按一级过程吸收,在11小时内产生相对恒定的血浆药物浓度。经皮吗啡的绝对生物利用度为75%(65 - 85%;95%置信区间)。经皮给药后M6G和M3G的血浆浓度均低于静脉输注后,且在代谢产物可检测到之前观察到相当长的延迟(长达1小时)。两种给药方式后,M3G和M6G相对于吗啡的AUC比值相似。4. 在经皮给药后观察到的较低血浆药物和代谢产物浓度下,非镇痛作用比静脉输注吗啡后不那么明显。5. 吗啡经皮给药作为一种替代的吗啡给药途径值得研究。
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