Department of Cardiology, Lund University Hospital, Lund, Sweden.
Thromb Haemost. 2010 Mar;103(3):604-12. doi: 10.1160/TH09-07-0509. Epub 2010 Jan 13.
AZD0837 is an investigational oral anticoagulant which is converted to the active form, AR-H067637, a selective direct thrombin inhibitor. The present study, a multicentre, randomised, parallel-group, dose-guiding study, assessed the safety and tolerability of an immediate-release formulation of AZD0837 compared with dose-adjusted warfarin in the prevention of stroke and systemic embolic events in atrial fibrillation (AF) patients. Two hundred fifty AF patients with at least one additional risk factor for stroke were randomised to receive either immediate-release AZD0837 (150mg twice daily [bid] or 350mg bid, blinded treatment) or dose-adjusted warfarin (international normalised ratio 2.0-3.0, open treatment) for three months. The safety and tolerability of 150mg bid AZD0837 appeared to be as good as that of warfarin. Total bleeding events were six with 150mg bid AZD0837, 15 with 350mg bid AZD0837 and eight with warfarin. Alanine aminotransferase elevations (>3xupper limit of normal) were infrequent, without apparent differences between treatment groups. A numerically higher incidence of serious adverse events was observed with 350mg bid AZD0837 compared with 150mg bid, with six of 13 being cardiac related, all with different diagnoses. An increase in mean serum creatinine of approximately 10% was observed in both AZD0837 groups, which returned to baseline after completion of therapy. There were no strokes, transient ischaemic attacks or cerebral haemorrhages with any of the treatments. In conclusion, the safety and tolerability of 150mg bid immediate-release AZD0837 appeared to be as good as that of dose-adjusted warfarin. However, larger studies will be needed to define the safety profile of AZD0837.
AZD0837 是一种研究性的口服抗凝剂,可转化为活性形式 AR-H067637,一种选择性的直接凝血酶抑制剂。本研究为一项多中心、随机、平行分组、剂量指导研究,旨在评估即刻释放型 AZD0837 与剂量调整华法林相比,在预防心房颤动 (AF) 患者中风和全身性栓塞事件方面的安全性和耐受性。250 例 AF 患者至少有一个中风的附加危险因素,随机接受即刻释放型 AZD0837(150mg 每日两次 [bid]或 350mg bid,盲法治疗)或剂量调整华法林(国际标准化比值 2.0-3.0,开放治疗)治疗 3 个月。150mg bid AZD0837 的安全性和耐受性似乎与华法林相当。共有 6 例出现 150mg bid AZD0837 出血事件,15 例出现 350mg bid AZD0837 出血事件,8 例出现华法林出血事件。丙氨酸氨基转移酶升高(>3x 正常值上限)不常见,各组间无明显差异。与 150mg bid 相比,350mg bid AZD0837 观察到严重不良事件发生率较高,其中 6 例与心脏相关,均有不同的诊断。在 AZD0837 两组中均观察到平均血清肌酐升高约 10%,治疗结束后恢复至基线。任何治疗均未发生中风、短暂性脑缺血发作或脑出血。总之,150mg bid 即刻释放型 AZD0837 的安全性和耐受性似乎与剂量调整华法林相当。然而,需要更大的研究来确定 AZD0837 的安全性概况。
