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Pharmacokinetics of gamma-hydroxybutyric acid in alcohol dependent patients after single and repeated oral doses.

机译:单次和重复口服剂量后酒精依赖型患者中γ-羟基丁酸的药代动力学。

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摘要

1. The pharmacokinetics of gamma-hydroxybutyric acid (GHB) were studied in 10 alcohol dependent subjects after single and repeated therapeutic oral doses (25 mg kg-1 every 12 h for 7 days). 2. GHB was readily absorbed and rapidly eliminated (tmax = 20-45 min; mean t1/2z 27 +/- 5 s.d. min). Urinary recovery of unchanged GHB was negligible (less than 1% of the dose). gamma-butyrolactone was not detected in either plasma or urine, indicating that lactonization of GHB does not occur in vivo. 3. The multiple-dose regimen resulted neither in accumulation of GHB nor in time-dependent modification of its pharmacokinetics. 4. In five subjects, the data were consistent with nonlinear elimination kinetics of GHB. Administration of a 50 mg kg-1 dose to these subjects resulted in significant increases in dose-normalized AUC, t1/2z and mean residence time. 5. Doubling of the dose also resulted in a significant increase in tmax with little change in Cmax. 6. At the administered doses, GHB did not accumulate in the plasma and caused no serious side effects.
机译:1.在单次和重复口服治疗(每12小时25 mg kg-1,共7天)后,在10位酒精依赖的受试者中研究了γ-羟基丁酸(GHB)的药代动力学。 2. GHB易于吸收并迅速消除(tmax = 20-45分钟;平均t1 / 2z 27 +/- 5 s.d.分钟)。尿中未改变的GHB的恢复可以忽略不计(少于剂量的1%)。在血浆或尿液中均未检测到γ-丁内酯,表明体内未发生GHB的内酯化。 3.多剂量方案既不导致GHB蓄积也不导致其药代动力学的时间依赖性改变。 4.在五个受试者中,数据与GHB的非线性消除动力学一致。给这些受试者服用50 mg kg-1剂量会导致剂量标准化的AUC,t1 / 2z和平均停留时间显着增加。 5.剂量加倍还导致tmax显着增加,而Cmax几乎没有变化。 6.在给药剂量下,GHB不会在血浆中积聚,也不会引起严重的副作用。

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