Verhoef J C, van den Wildenberg H M
Regul Pept. 1986 Apr;14(2):113-24. doi: 10.1016/0167-0115(86)90212-0.
A pharmacokinetic study with [3H]des-enkephalin-gamma-endorphin (3H-DE gamma E) was performed in rats after the intravenous, subcutaneous and intramuscular route of administration. Disappearance of non-metabolized 3H-DE gamma E from blood upon intravenous dosing followed a biphasic decay with half-lives of 0.7 +/- 0.3 (+/- S.D.) min for the initial distribution phase and 6.3 +/- 2.7 min for the terminal elimination phase. The central and peripheral volumes of distribution were strikingly high (0.38 and 0.55 1 X kg-1, respectively). Extensive metabolism occurred already within the first minutes after injection. The blood clearance rate was found to be 0.29 +/- 0.12 1 X min-1 X kg-1, which value points to remarkable extrahepatic elimination of the neuropeptide. As compared to the intravenous route of administration, subcutaneous or intramuscular injection of 3H-DE gamma E resulted in low but longer-lasting peptide levels in blood. These levels reached already peak values at 2 min after both routes of administration and then declined to below the limit of detection at 2-3 h. The absolute bioavailability of DE gamma E after subcutaneous injection amounted to 30.9 +/- 16.3% (range 16.0-46.9%), whereas the bioavailability after intramuscular injection was observed to be 3.5 times lower (8.5 +/- 3.0%; range 4.6-12.0%). These data suggest that subcutaneous dosing of DE gamma E might be more effective in displaying CNS activity than the intramuscular route.
对大鼠进行了静脉内、皮下和肌肉内注射[3H]去甲脑啡肽-γ-内啡肽(3H-DEγE)后的药代动力学研究。静脉给药后,血液中未代谢的3H-DEγE的消失呈双相衰减,初始分布相的半衰期为0.7±0.3(±标准差)分钟,终末消除相的半衰期为6.3±2.7分钟。中央和外周分布容积显著较高(分别为0.38和0.55升/千克)。注射后最初几分钟内就发生了广泛的代谢。发现血液清除率为0.29±0.12升/分钟·千克,该值表明该神经肽有显著的肝外消除。与静脉给药途径相比,皮下或肌肉内注射3H-DEγE导致血液中肽水平较低但持续时间较长。两种给药途径后,这些水平在2分钟时已达到峰值,然后在2-3小时时降至检测限以下。皮下注射后DEγE的绝对生物利用度为30.9±16.3%(范围16.0-46.9%),而肌肉内注射后的生物利用度观察到低3.5倍(8.5±3.0%;范围4.6-12.0%)。这些数据表明,皮下给药DEγE在显示中枢神经系统活性方面可能比肌肉内给药途径更有效。
