Department of Clinical Pharmacology, Idorsia Pharmaceuticals Ltd., Allschwil 4123, Switzerland.
Quintiles Drug Research Unit, London SE1 1YR, UK.
Int J Mol Sci. 2017 Dec 6;18(12):2636. doi: 10.3390/ijms18122636.
The pharmacokinetics, pharmacodynamics, tolerability, and food effect of cenerimod, a potent sphingosine-1-phosphate subtype 1 receptor modulator, were investigated in three sub-studies. Two double-blind, placebo-controlled, randomised studies in healthy male subjects were performed. Cenerimod was administered either as single dose (1, 3, 10 or 25 mg; Study 1) or once daily for 35 days (0.5, 1, 2 or 4 mg; Study 2). A two-period cross-over, open-label study was performed to assess the food effect (1 mg, Study 3). The pharmacokinetic profile of cenerimod was characterised by a of 5.0-6.2 h. Terminal half-life after single and multiple doses ranged from 170 to 199 h and 283 to 539 h, respectively. Food had no relevant effect on the pharmacokinetics of cenerimod. A dose-dependent decrease in lymphocyte count was observed after initiation of cenerimod and reached a plateau (maximum change from baseline: -64%) after 20-23 days of treatment. Lymphocyte counts returned to baseline values at end-of-study examination. One serious adverse event of circulatory collapse (25 mg dose group, maximum tolerated dose: 10 mg) and adverse events of mild-to-moderate intensity were reported. Treatment initiation was associated with transient decreases in heart rate and blood pressure at doses >1 and ≥10 mg, respectively.
在三项子研究中考察了 cenerimod 的药代动力学、药效学、耐受性和食物效应。这是两项在健康男性受试者中进行的双盲、安慰剂对照、随机研究。cenerimod 分别以单剂量(1、3、10 或 25mg;研究 1)或每日一次给药(0.5、1、2 或 4mg;研究 2)给药 35 天。一项两周期交叉、开放标签研究用于评估食物效应(研究 3)。cenerimod 的药代动力学特征为 5.0-6.2 小时。单剂量和多剂量后的终末半衰期范围分别为 170-199 小时和 283-539 小时。食物对 cenerimod 的药代动力学无显著影响。在开始使用 cenerimod 后观察到淋巴细胞计数呈剂量依赖性下降,并在治疗 20-23 天后达到平台期(与基线相比最大变化:-64%)。在研究结束时,淋巴细胞计数恢复到基线值。报告了一例严重不良事件(循环衰竭,25mg 剂量组,最大耐受剂量:10mg)和轻度至中度强度的不良事件。在剂量>1 和≥10mg 时,治疗开始与心率和血压的短暂下降相关。
Zotero 插件
