GlaxoSmithKline, Research Triangle Park, NC 27709, USA.
J Clin Pharmacol. 2013 Sep;53(9):955-61. doi: 10.1002/jcph.127. Epub 2013 Jul 12.
Dabrafenib is an orally bioavailable, potent, and selective inhibitor of human wild-type BRAF and CRAF kinases as well as mutant forms of BRAF kinase. The aim of this phase 1, single-center, open-label study in four patients with BRAF mutation-positive solid tumors was to determine the absolute bioavailability of a 150 mg oral dose of dabrafenib. A microtracer study approach, in which a 50 µg radiolabeled intravenous (IV) microdose of dabrafenib was given concomitantly with a 150 mg oral dose, was used to simultaneously recover IV and oral pharmacokinetic parameters. The least squares mean (90% CI) absolute bioavailability of dabrafenib (HPMC capsules) was 94.5% (81.3%, 109.7%). Median T(max) after oral administration was 2.0 hours and the geometric mean terminal half-life was 4.8 hours. The geometric mean clearance and volume of distribution after IV administration were 12.0 L/h and 45.5 L, respectively. Human clearance and volume of distribution at steady state were in agreement with predictions made using allometric scaling of pharmacokinetic parameters from four preclinical species. In conclusion, dabrafenib absolute bioavailability was high, whereas first-pass metabolism was low. Furthermore, the microtracer approach provided an innovative and efficient method for assessing the absolute bioavailability of dabrafenib in patients with advanced cancer.
达布拉非尼是一种口服生物利用度高、强效且选择性的人源野生型 BRAF 和 CRAF 激酶以及 BRAF 激酶突变体抑制剂。本研究是一项在 4 例 BRAF 突变阳性实体瘤患者中进行的 1 期、单中心、开放性研究,旨在确定 150mg 口服剂量达布拉非尼的绝对生物利用度。采用微示踪剂研究方法,即同时给予 50μg 放射性标记的静脉(IV)微剂量达布拉非尼和 150mg 口服剂量,同时回收 IV 和口服药代动力学参数。达布拉非尼(HPMC 胶囊)的最低平方均值(90%CI)绝对生物利用度为 94.5%(81.3%,109.7%)。口服给药后中位数 Tmax 为 2.0 小时,几何均数终末半衰期为 4.8 小时。IV 给药后的几何平均清除率和分布容积分别为 12.0 L/h 和 45.5 L。人在稳态时的清除率和分布容积与通过种属间外推法预测的药代动力学参数一致。总之,达布拉非尼的绝对生物利用度较高,而首过代谢率较低。此外,微示踪剂研究方法为评估晚期癌症患者达布拉非尼的绝对生物利用度提供了一种创新且高效的方法。
