咪达唑仑及α-羟基咪达唑仑经直肠和静脉给药后的药代动力学
Pharmacokinetics of midazolam and alpha-hydroxy-midazolam following rectal and intravenous administration.
作者信息
Clausen T G, Wolff J, Hansen P B, Larsen F, Rasmussen S N, Dixon J S, Crevoisier C
机构信息
Department of Anaesthesia, Bispebjerg Hospital, Copenhagen, Denmark.
出版信息
Br J Clin Pharmacol. 1988 Apr;25(4):457-63. doi: 10.1111/j.1365-2125.1988.tb03330.x.
Abstract
- In an open cross-over trial, plasma concentrations of midazolam were measured in eight healthy male volunteers following administration of 0.3 mg kg-1 body weight given by the rectal and intravenous routes. 2. Maximum plasma concentrations of 92-156 ng ml-1 (mean 118 ng ml-1) were recorded from 20 to 50 min (mean 31 min) after rectal application. The rectal bioavailability was 40-65% (mean 52%) and the terminal half-life was 114-305 min (mean 161 min). 3. A substantial first-pass hepatic effect was observed following rectal administration. 4. No systemic or local intolerance was noted. 5. In conclusion, the rectal route of administration provides a rapid and reliable absorption of midazolam.
摘要
- 在一项开放性交叉试验中,对8名健康男性志愿者经直肠和静脉途径给予0.3毫克/千克体重的咪达唑仑后,测量其血浆浓度。2. 直肠给药后20至50分钟(平均31分钟)记录到的最大血浆浓度为92 - 156纳克/毫升(平均118纳克/毫升)。直肠生物利用度为40% - 65%(平均52%),终末半衰期为114 - 305分钟(平均161分钟)。3. 直肠给药后观察到显著的首过肝效应。4. 未发现全身或局部不耐受情况。5. 总之,直肠给药途径能使咪达唑仑快速且可靠地吸收。
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