Laskin O L, Longstreth J A, Hart C C, Scavuzzo D, Kalman C M, Connor J D, Roberts R B
Clin Pharmacol Ther. 1987 May;41(5):546-55. doi: 10.1038/clpt.1987.70.
Ribavirin is a broad-spectrum antiviral drug that has in vitro activity against human immunodeficiency virus. To determine the kinetics of ribavirin, 17 symptom-free homosexual men with lymphadenopathy were studied. Single doses of ribavirin, 600, 1200, or 2400 mg, were given orally or intravenously. The plasma ribavirin concentration-time profiles were well fitted by a three-compartment open model. Ribavirin followed linear kinetics over the dose range studied. The mean 1-hour postinfusion concentrations after intravenous ribavirin, 600, 1200, and 2400 mg, were 8.0, 19.7, and 37.1 mumol/L, respectively. The mean +/- SD plasma beta-phase half-life, terminal-phase (gamma) half-life, and volume of distribution at steady state were 2.0 +/- 1.1 hours, 35.5 +/- 14.0 hours, and 647 +/- 258 L, respectively. The mean ribavirin renal clearance and total body clearance were 99 +/- 30 and 283 +/- 37 ml/min, respectively. After an oral dose of 600, 1200, and 2400 mg, the mean peak plasma ribavirin concentrations (which occurred 1.5 hours after administration) were 5.1, 9.9, and 12.6 mumol/L, respectively. The mean absorption half-life and bioavailability of ribavirin were 0.5 hour and 45%. Ribavirin had no plasma protein binding and the drug accumulated within red blood cells. In conclusion, ribavirin is incompletely absorbed from the gastrointestinal tract, its renal excretion accounts for approximately one third of the drug's elimination, and drug accumulation (greater than threefold) will result with repetitive dosing at the 6- to 8-hour dosing interval currently used.
利巴韦林是一种具有抗人免疫缺陷病毒体外活性的广谱抗病毒药物。为了确定利巴韦林的动力学,对17名无症状的有淋巴结病的同性恋男性进行了研究。口服或静脉给予单剂量600、1200或2400mg的利巴韦林。血浆利巴韦林浓度-时间曲线用三室开放模型拟合良好。在所研究的剂量范围内,利巴韦林遵循线性动力学。静脉注射600、1200和2400mg利巴韦林后1小时的平均血药浓度分别为8.0、19.7和37.1μmol/L。平均±标准差的血浆β相半衰期、终末相(γ)半衰期和稳态分布容积分别为2.0±1.1小时、35.5±14.0小时和647±258L。利巴韦林的平均肾清除率和全身清除率分别为99±30和283±37ml/min。口服600、1200和2400mg剂量后,平均血浆利巴韦林峰浓度(给药后1.5小时出现)分别为5.1、9.9和12.6μmol/L。利巴韦林的平均吸收半衰期和生物利用度分别为0.5小时和45%。利巴韦林不与血浆蛋白结合,且药物在红细胞内蓄积。总之,利巴韦林从胃肠道吸收不完全,其经肾排泄约占药物消除的三分之一,按目前6至8小时的给药间隔重复给药会导致药物蓄积(大于三倍)。
