Christopher Ronald, Covington Paul, Davenport Michael, Fleck Penny, Mekki Qais A, Wann Elisabeth R, Karim Aziz
Takeda San Diego, Inc., San Diego, California 92121, USA.
Clin Ther. 2008 Mar;30(3):513-27. doi: 10.1016/j.clinthera.2008.03.005.
Alogliptin is a highly selective dipeptidyl peptidase-4 (DPP-4) inhibitor that is under development for the treatment of type 2 diabetes.
This study was conducted to characterize the pharmacokinetics, pharmacodynamics, and tolerability of single oral doses of alogliptin in healthy male subjects.
This was a randomized, double-blind, placebo-controlled study in which healthy, nonobese male subjects between the ages of 18 and 55 years were assigned to 1 of 6 cohorts: alogliptin 25, 50, 100, 200, 400, or 800 mg. One subject in each cohort received placebo. An ascending-dose strategy was used, in which each cohort received its assigned dose only after review of the safety data from the previous cohort. Blood and urine were collected over 72 hours after dosing for pharmacokinetic analysis and determination of plasma DPP-4 inhibition and active glucagon-like peptide -1(GLP-1) concentrations.
Thirty-six subjects (66 per cohort) were enrolled and completed the study (29/36 [81% ] white; mean age, 26.6 years; mean weight, 76.0 kg). Alogliptin was rapidly absorbed (median T(max), 1-2 hours) and eliminated slowly (mean t(1/2), 12.4-21.4 hours), primarily via urinary excretion (mean fraction of drug excreted in urine from 0 to 72 hours after dosing, 60%-71%). C(max) and AUC(0-infinity) increased dose proportionally over the range from 25 to 100 mg. The metabolites M-I (N-demethylated) and M-II (N-acetylated) accounted for <2% and <6%, respectively, of alogliptin concentrations in plasma and urine. Across alogliptin doses, mean peak DPP-4 inhibition ranged from 93% to 99%, and mean inhibition at 24 hours after dosing ranged from 74% to 97%. Exposure to active GLP-1 was 2- to 4-fold greater for all alogliptin doses compared with placebo; no dose response was apparent. Hypoglycemia (asymptomatic) was reported in 5 subjects (11 receiving alogliptin 50 mg, 2 receiving alogliptin 200 mg, 1 receiving alogliptin 400 mg, 1 receiving placebo). Other adverse events were reported in 1 subject each: dizziness (alogliptin 100 mg), syncope (alogliptin 200 mg), constipation (alogliptin 200 mg), viral infection (alogliptin 400 mg), hot flush (placebo), and nausea (placebo).
In these healthy male subjects, alogliptin at single doses up to 800 mg inhibited plasma DPP-4 activity, increased active GLP-1, and was generally well tolerated, with no dose-limiting toxicity.
阿格列汀是一种高选择性二肽基肽酶-4(DPP-4)抑制剂,正处于治疗2型糖尿病的研发阶段。
本研究旨在描述健康男性受试者单次口服阿格列汀的药代动力学、药效动力学及耐受性。
这是一项随机、双盲、安慰剂对照研究,将18至55岁健康、非肥胖男性受试者分为6个队列之一:阿格列汀25、50、100、200、400或800 mg。每个队列中有1名受试者接受安慰剂。采用递增剂量策略,即每个队列仅在审查前一个队列的安全性数据后才接受其指定剂量。给药后72小时内采集血液和尿液进行药代动力学分析,并测定血浆DPP-4抑制率及活性胰高血糖素样肽-1(GLP-1)浓度。
36名受试者(每个队列6名)入组并完成研究(29/36 [81%]为白人;平均年龄26.6岁;平均体重76.0 kg)。阿格列汀吸收迅速(中位达峰时间T(max)为1 - 2小时),消除缓慢(平均半衰期t(1/2)为12.4 - 21.4小时),主要通过尿液排泄(给药后0至72小时尿液中排泄的药物平均比例为60% - 71%)。在25至100 mg范围内,C(max)和AUC(0 - ∞)与剂量成比例增加。代谢产物M-I(N-去甲基化)和M-II(N-乙酰化)分别占血浆和尿液中阿格列汀浓度的<2%和<6%。在所有阿格列汀剂量下,平均DPP-4抑制峰值范围为93%至99%,给药后24小时的平均抑制率范围为74%至97%。与安慰剂相比,所有阿格列汀剂量下活性GLP-1的暴露量高2至4倍;未观察到明显的剂量反应。5名受试者报告有低血糖(无症状)(11名接受阿格列汀50 mg,2名接受阿格列汀200 mg,1名接受阿格列汀400 mg,1名接受安慰剂)。其他不良事件各有1名受试者报告:头晕(阿格列汀100 mg)、晕厥(阿格列汀200 mg)、便秘(阿格列汀200 mg)、病毒感染(阿格列汀400 mg)、潮热(安慰剂)和恶心(安慰剂)。
在这些健康男性受试者中,单次剂量高达800 mg的阿格列汀可抑制血浆DPP-4活性,增加活性GLP-1,且总体耐受性良好,无剂量限制毒性。
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