A Phase 1, Open-Label Study in Healthy Subjects to Evaluate the Absolute Bioavailability of AG-221 by a Microtracer Approach

Xiaomin Wang; Jian Chen; Josephine Reyes; Simon Zhou; Maria Palmisano; Yan Li

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IntroductionThe purpose of this study was to evaluate the absolute bioavailability (BA) of AG-221 following a single oral dose of 100?mg AG-221 and an intravenous (IV) dose of?~?100?μg AG-221 containing approximately 300 nCi of [ 14 C]-AG-221.MethodsThis was a phase 1, open-label study. Six subjects who met all of the inclusion criteria and none of the exclusion criteria were enrolled in the study. After an overnight fast of at least 10?h, the subjects received an oral dose (coated tablet) of 100?mg of AG-221 at 0?h on dosing day. Four hours after the oral dose, the subjects received 100?μg AG-221 containing?~?300 nCi of [ 14 C]-AG-221 administered as an IV bolus. Blood samples were collected and analyzed for plasma concentrations of AG-221 and [ 14 C]-AG-221 using a validated liquid chromatography with tandem mass spectrometry (LC–MS/MS) system and high-performance liquid chromatography (HPLC) fractionation followed by accelerator mass spectrometry analysis (AMS), respectively. Safety was evaluated throughout the study.ResultsThe absolute BA after a 100-mg oral dose of AG-221 was measured as 57.2%. While the total clearance was 1.37 L/h,?~?1/60 of the liver blood flow in a typical 70-kg human subject, the first-pass extraction was estimated to be less than 2%, assuming that the total clearance was entirely due to liver metabolism. Thus, the fraction of the AG-221 dose absorbed was at least 50%. AG-221 was safe and well tolerated when given under fasted conditions in a single 100-mg dose as a coated tablet with a microtracer [ 14 C]-AG-221 solution, as few drug-related treatment-emergent adverse events (TEAEs) were reported. No clinically significant changes or findings were noted in the clinical laboratory evaluations, vital sign measurements, and electrocardiograms (ECGs) performed during this study.ConclusionsIn healthy subjects under fasting conditions, the absolute BA following oral administration of a 100-mg AG-221 tablet was 57.2%. AG-221 was safe and well tolerated in healthy male subjects when administered as a single 100-mg film-coated tablet plus 100?μg [ 14 C]-AG-221 given intravenously.Trial RegistrationClinicalTrials.gov identifier, NCT02443168.FundingCelgene Corporation.

机译：介绍该研究的目的是评估单个口服剂量100〜Mg Ag-221和静脉内（IV）剂量的Ag-221的绝对生物利用度（BA），含有约300的静脉内（IV）剂量的α〜100？μgAg-221 [14 c] -ag-221.Methodsthis的NCI是1阶段，开放标签研究。符合所有纳入标准的六个受试者和任何排除标准都在研究中进行了纳入。在过夜至少10℃的过夜后，受试者在剂量天时间接受100μmg-221的100μmg-221的口服剂量（涂覆片剂）。口服剂量4小时后，受试者收到100≤μg-221的[14 c] -221作为IV推注300 NCI。使用验证的液相色谱法收集并分析血浆浓度的血浆浓度和[14c] -Ag-221，验证的液相色谱法与串联质谱（LC-MS / MS）系统和高效液相色谱（HPLC）分馏。随后通过加速器质谱分析（AMS）。在整个研究中评估了安全性。在100mg口服剂量的Ag-221后，测量为57.2％后的绝对BA。虽然总关算为1.37升/小时，但β1/60在典型的70kg人体受试者中，首先萃取率估计小于2％，假设总清除量是完全是由于肝脏代谢。因此，Ag-221剂量的级分吸收至少为50％。当在单个100mg剂量的禁食条件下作为涂层片剂的禁食条件给出时，Ag-221是安全且耐受性的，作为涂层的片剂[14 c] -ag-221溶液，少量药物相关治疗 - 紧急不良事件（茶）据报道。在本研究期间，在临床实验室评估，生命符号测量和心电图（ECG）中没有注意到临床上显着的变化或发现。在禁食条件下的健康受试者，口服施用100mg AG-221片剂后的绝对BA 57.2％。当静脉内施用时，Ag-221在健康的男性受试者中，在健康的男性受试者中是安全的，并且在静脉内施用的单个100mg膜涂层片剂加上100μgαμg[14 c] -ag-221 .Tirdclealclinictrials.gov标识符，NCT02443168.FundingCelgene Corporation。

A Phase 1, Open-Label Study in Healthy Subjects to Evaluate the Absolute Bioavailability of AG-221 by a Microtracer Approach

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