Harrison Lester I, Astry Calvin, Kumar Sandeep, Yunis Carla
Department of Pharmacokinetics/Drug Metabolism, 3M Pharmaceuticals, Center Bldg 270-3S-05, St Paul, MN 55144, USA.
J Clin Pharmacol. 2007 Aug;47(8):962-9. doi: 10.1177/0091270007303766.
852A is an imidazoquinoline Toll-like receptor 7 agonist undergoing evaluation for the systemic treatment of cancer. 852A was administered to 6 healthy subjects as 3 rising subcutaneous doses (0.5 to 1.0 to 2.0 mg), to 6 subjects as 3 oral doses (10.0 to 20.0 to 15.0 mg, the third dose being a de-escalation), and to 6 subjects as a 2.0-mg dose by the subcutaneous, intravenous, and oral routes in crossover fashion. The subcutaneous and intravenous doses were well tolerated. One subject withdrew following the 20.0-mg oral dose because of hypotension. The 2.0-mg subcutaneous dose had 80.5% +/- 12.8% (mean +/- SD) bioavailability and gave serum concentrations comparable to intravenous administration by 30 minutes. Linear kinetics and an interferon-alpha dose response were observed for the 3 subcutaneous doses. Serum concentrations following the 2.0-mg oral dose were always lower than those following the same intravenous dose, and the oral route had a bioavailability of 26.5% +/- 7.84%. Concentrations appeared to increase with oral dose; however, large variabilities in both the rate and extent of absorption were seen between individuals. Approximately 40% of an absorbed dose was excreted unchanged in the urine. Overall, the study suggests that subcutaneous administration may be an acceptable method to deliver 852A for systemic applications.
852A是一种咪唑喹啉类Toll样受体7激动剂,正在进行癌症全身治疗的评估。852A以3个递增的皮下剂量(0.5至1.0至2.0毫克)给予6名健康受试者,以3个口服剂量(10.0至20.0至15.0毫克,第三剂为递减剂量)给予6名受试者,并以交叉方式通过皮下、静脉和口服途径给予6名受试者2.0毫克剂量。皮下和静脉剂量耐受性良好。一名受试者在口服20.0毫克剂量后因低血压退出。2.0毫克皮下剂量的生物利用度为80.5%±12.8%(平均值±标准差),30分钟时血清浓度与静脉给药相当。观察到3个皮下剂量呈线性动力学和干扰素-α剂量反应。口服2.0毫克剂量后的血清浓度始终低于相同静脉剂量后的血清浓度,口服途径的生物利用度为26.5%±7.84%。浓度似乎随口服剂量增加;然而,个体之间在吸收速率和程度上均存在较大差异。约40%的吸收剂量以原形从尿液中排泄。总体而言,该研究表明皮下给药可能是全身应用852A的一种可接受的给药方法。
