两项 1 期、开放性、物质平衡研究,旨在确定健康男性志愿者中 C 标记的硫酸异帕米星的药代动力学。
Two Phase 1, Open-Label, Mass Balance Studies to Determine the Pharmacokinetics of C-Labeled Isavuconazonium Sulfate in Healthy Male Volunteers.
机构信息
Astellas Pharma Global Development Inc., Northbrook, IL, USA.
Analysis & Pharmacokinetics Research Laboratories, Astellas Pharma Inc, Osaka, Japan.
出版信息
Clin Pharmacol Drug Dev. 2018 Feb;7(2):207-216. doi: 10.1002/cpdd.376. Epub 2017 Jul 27.
Isavuconazonium sulfate is the water-soluble prodrug of the active triazole isavuconazole. Two phase 1 studies were conducted to identify the metabolic profile and mass balance of isavuconazole and BAL8728 (inactive cleavage product). Seven subjects in study 1 (isavuconazole mass balance) received a single oral dose of [cyano- C]isavuconazonium sulfate corresponding to 200 mg isavuconazole. Six subjects in study 2 (BAL8728 mass balance) received a single intravenous dose of [pyridinylmethyl- C]isavuconazonium sulfate corresponding to 75 mg BAL8728. Pharmacokinetic parameters of radioactivity in whole blood and plasma and of isavuconazole and BAL8728 in plasma were assessed. Radioactivity ratio of blood/plasma, percentage of dose, and cumulative percentage of radioactive dose recovered in urine and feces for isavuconazole and BAL8728 were assessed. Metabolic profiling was carried out by high-performance liquid chromatography and mass spectrometry. Mean plasma isavuconazole pharmacokinetic parameters included apparent clearance (2.3 ± 0.7 L/h), apparent volume of distribution (301.8 ± 105.7 L), and terminal elimination half-life (99.9 ± 44.6 hours). In study 1, isavuconazole-derived radioactivity was recovered approximately equally in urine and feces (46.1% and 45.5%, respectively). In study 2, BAL8728-derived radioactivity was predominantly recovered in urine (96.0%). Isavuconazole (study 1) and M4 (cleavage metabolite of BAL8728; study 2) were the predominant circulating components of radioactivity in plasma.
硫酸伊曲康唑是活性三唑伊曲康唑的水溶性前药。进行了两项 I 期研究以确定伊曲康唑和 BAL8728(无活性裂解产物)的代谢特征和质量平衡。在研究 1(伊曲康唑质量平衡)中,7 名受试者单次口服[氰基- C]伊曲康唑硫酸盐,相当于 200mg 伊曲康唑。在研究 2(BAL8728 质量平衡)中,6 名受试者单次静脉注射[吡啶甲基- C]伊曲康唑硫酸盐,相当于 75mg BAL8728。评估了全血和血浆中放射性的药代动力学参数以及血浆中伊曲康唑和 BAL8728 的药代动力学参数。评估了伊曲康唑和 BAL8728 的血/血浆放射性比、剂量百分比和尿液和粪便中放射性剂量的累积百分比。通过高效液相色谱和质谱进行代谢特征分析。伊曲康唑的平均血浆药代动力学参数包括表观清除率(2.3±0.7 L/h)、表观分布容积(301.8±105.7 L)和终末消除半衰期(99.9±44.6 小时)。在研究 1 中,伊曲康唑衍生的放射性物质大约等量地在尿液和粪便中回收(分别为 46.1%和 45.5%)。在研究 2 中,BAL8728 衍生的放射性物质主要在尿液中回收(96.0%)。伊曲康唑(研究 1)和 M4(BAL8728 的裂解代谢物;研究 2)是血浆中放射性的主要循环成分。
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