GlaxoSmithKline, 709 Swedeland Road, King of Prussia, PA 19406, USA.
Br J Clin Pharmacol. 2013 Jul;76(1):99-106. doi: 10.1111/bcp.12063.
The purpose of this study was to establish safety and tolerability of a single intravenous (IV) infusion of a p38 mitogen-activated protein kinase inhibitor, losmapimod, to obtain therapeutic levels rapidly for a potential acute coronary syndrome indication. Pharmacokinetics (PK) following IV dosing were characterized, and pharmacokinetic/pharmacodynamic (PK/PD) relationships between losmapimod and phosphorylated heat shock protein 27 (pHSP27) and high-sensitivity C-reactive protein were explored.
Healthy volunteers received 1 mg losmapimod IV over 15 min (n = 4) or 3 mg IV over 15 min followed by a washout period and then 15 mg orally (PO; n = 12). Pharmacokinetic parameters were calculated by noncompartmental methods. The PK/PD relationships were explored using modelling and simulation.
There were no deaths, nonfatal serious adverse events or adverse events leading to withdrawal. Headache was the only adverse event reported more than once (n = 3 following oral dosing). Following 3 mg IV and 15 mg PO, Cmax was 59.4 and 45.9 μg l(-1) and AUC0-∞ was 171.1 and 528.0 μg h l(-1) , respectively. Absolute oral bioavailability was 0.62 [90% confidence interval (CI) 0.56, 0.68]. Following 3 mg IV and 15 mg PO, maximal reductions in pHSP27 were 44% (95% CI 38%, 50%) and 55% (95% CI 50%, 59%) occurring at 30 min and 4 h, respectively. There was a 17% decrease (95% CI 9%, 24%) in high-sensitivity C-reactive protein 24 h following oral dosing. A direct-link maximal inhibitory effect model related plasma concentrations to pHSP27 concentrations.
A single IV infusion of losmapimod in healthy volunteers was safe and well tolerated, and may potentially serve as an initial loading dose in acute coronary syndrome as rapid exposure is achieved.
本研究旨在确定 p38 丝裂原活化蛋白激酶抑制剂洛索洛芬静脉(IV)输注单次给药的安全性和耐受性,以便快速获得治疗水平,用于潜在的急性冠脉综合征适应证。对 IV 给药后的药代动力学(PK)进行了特征描述,并探索了洛索洛芬与磷酸化热休克蛋白 27(pHSP27)和高敏 C 反应蛋白之间的药代动力学/药效动力学(PK/PD)关系。
健康志愿者静脉输注 1 毫克洛索洛芬 15 分钟(n = 4)或 3 毫克洛索洛芬 15 分钟,然后进行洗脱期,再口服 15 毫克(n = 12)。采用非房室模型法计算药代动力学参数。采用建模和模拟方法探讨 PK/PD 关系。
无死亡、非致命性严重不良事件或导致停药的不良事件。仅报告了 1 次以上的不良反应(口服给药后 n = 3),即头痛。静脉输注 3 毫克和口服 15 毫克后,Cmax 分别为 59.4 和 45.9 μg l(-1),AUC0-∞分别为 171.1 和 528.0 μg h l(-1)。绝对口服生物利用度为 0.62 [90%置信区间(CI)0.56,0.68]。静脉输注 3 毫克和口服 15 毫克后,pHSP27 的最大降幅分别为 44%(95%CI 38%,50%)和 55%(95%CI 50%,59%),分别发生在 30 分钟和 4 小时。口服给药后 24 小时,高敏 C 反应蛋白下降 17%(95%CI 9%,24%)。一个直接链接最大抑制效应模型将血浆浓度与 pHSP27 浓度相关联。
在健康志愿者中单次静脉输注洛索洛芬安全且耐受性良好,可能作为急性冠脉综合征的初始负荷剂量,因为可快速达到暴露水平。
