Yuen G J, Morris D M, Mydlow P K, Haidar S, Hall S T, Hussey E K
Department of Clinical Pharmacology, Glaxo Research Institute, Research Triangle Park, North Carolina 27709, USA.
J Clin Pharmacol. 1995 Dec;35(12):1174-80. doi: 10.1002/j.1552-4604.1995.tb04043.x.
Lamivudine is a novel cytosine nucleoside analog, reverse transcriptase inhibitor that has shown activity against human immunodeficiency virus (HIV) types 1 and 2 and hepatitis B virus in vitro. This study was conducted to compare the absolute bioavailability, pharmacokinetics, and absorption characteristics of oral solution, 100-mg capsule, and 100-mg tablet formulations of lamivudine with those of intravenous lamivudine. Twelve patients with HIV were enrolled in a single-center, randomized, open-label, four-way cross-over study. Treatment arms consisted of 100 mg intravenous lamivudine (administered over 1 hour), 100 mg oral lamivudine (1 mg/mL), a 100-mg capsule, and a 100-mg tablet, each followed by a 3- to 14-day washout period. Serial blood samples over 24 hours were obtained after each dose administration. Serum concentration data were analyzed to determine pharmacokinetic parameter estimates including area under the curve (AUC), terminal half-life (t1/2), mean residence time (MRT) for each formulation, systemic clearance, oral clearance, and apparent volume of distribution (Vd). Absolute bioavailability and in vivo mean absorption time (MAT) and mean dissolution time (MDT) were calculated for the oral formulations. Deconvolution techniques were used to calculate the input rate for the oral solution, capsule, and tablet. The two one-sided t test was used to determine bioequivalency among oral formulations with respect to logarithmic transformed estimates of AUC and maximum peak concentration (Cmax). Mean (CV) systemic clearance and Vdss after intravenous administration of lamivudine were 22.6 L/h (15%) and 99 L (28%), respectively; mean t1/2 ranged from 8.41 to 9.11 hours for all formulations; and MRT ranged from 4.42 to 5.77 hours for all formulations. Mean absolute bioavailability ranged from 86% to 88% for the oral solution, capsule, and tablet. All oral formulations were considered bioequivalent for AUC and Cmax. The MAT was 1.32 hour for the oral solution, and MDT was 0.03 and -0.11 hours for the capsule and the oral solution, respectively. The oral formulations of lamivudine examined in this study demonstrated acceptable bioavailability for oral administration. The solid oral formulations (capsule and tablet) show rapid dissolution properties with an absorption rate similar to or exceeding those observed with the oral solution. This suggests that dissolution is not an important factor for the rate of absorption of lamivudine. The use of deconvolution techniques using PCDCON provides valuable insight into the absorption characteristics of lamivudine.
拉米夫定是一种新型胞嘧啶核苷类似物,即逆转录酶抑制剂,已在体外显示出对1型和2型人类免疫缺陷病毒(HIV)以及乙型肝炎病毒的活性。本研究旨在比较拉米夫定口服溶液、100毫克胶囊和100毫克片剂制剂与静脉注射拉米夫定的绝对生物利用度、药代动力学和吸收特性。12名HIV患者参与了一项单中心、随机、开放标签、四交叉研究。治疗组包括100毫克静脉注射拉米夫定(1小时内给药)、100毫克口服拉米夫定(1毫克/毫升)、100毫克胶囊和100毫克片剂,每组给药后均有3至14天的洗脱期。每次给药后24小时内采集系列血样。分析血清浓度数据以确定药代动力学参数估计值,包括每种制剂的曲线下面积(AUC)、末端半衰期(t1/2)、平均驻留时间(MRT)、全身清除率、口服清除率和表观分布容积(Vd)。计算口服制剂的绝对生物利用度以及体内平均吸收时间(MAT)和平均溶解时间(MDT)。采用反卷积技术计算口服溶液、胶囊和片剂的输入速率。采用双向单侧t检验确定口服制剂在AUC和最大峰浓度(Cmax)对数转换估计值方面的生物等效性。静脉注射拉米夫定后的平均(CV)全身清除率和稳态分布容积分别为22.6升/小时(15%)和99升(28%);所有制剂的平均t1/2范围为8.41至9.11小时;所有制剂的MRT范围为4.42至5.77小时。口服溶液、胶囊和片剂的平均绝对生物利用度范围为86%至88%。所有口服制剂在AUC和Cmax方面均被认为具有生物等效性。口服溶液的MAT为1.32小时,胶囊和口服溶液的MDT分别为0.03和 -0.11小时。本研究中检测的拉米夫定口服制剂显示出可接受的口服生物利用度。固体口服制剂(胶囊和片剂)显示出快速溶解特性,吸收速率与口服溶液相似或超过口服溶液。这表明溶解不是拉米夫定吸收速率的重要因素。使用PCDCON的反卷积技术为拉米夫定的吸收特性提供了有价值的见解。
