Müller T H, Weisenberger H, Brickl R, Narjes H, Himmelsbach F, Krause J
Department of Biological Research, Dr Karl Thomae GmbH, Biberach, Germany.
Circulation. 1997 Aug 19;96(4):1130-8. doi: 10.1161/01.cir.96.4.1130.
Clinical trials have demonstrated that platelet glycoprotein (GP) IIb/IIIa antagonists effectively prevent acute thrombotic events. Orally active GP IIb/IIIa antagonists are essential to evaluate the clinical benefit of long-term treatment. We therefore investigated platelet inhibition by the GP IIb/IIIa antagonist Fradafiban (BIBU 52; Fradafiban is the recommended INN of BIBU 52) and its orally administered prodrug, Lefradafiban (BIBU 104; Lefradafiban is the recommended INN of BIBU 104) in healthy subjects.
The activity and plasma levels of Fradafiban and Lefradafiban were evaluated in double-blind, placebo-controlled studies in 130 healthy male subjects. One to 15 mg Fradafiban continuously infused over 30 minutes reversibly inhibited platelet aggregation in platelet-rich plasma ex vivo in response to 20 micromol/L ADP (5 mg, 100% inhibition at 27 minutes after administration) and to both 1.0 (5 mg, 100%) and 10 microg/mL (15 mg, 97+/-3%) collagen. Single oral doses of Lefradafiban inhibited ADP-induced aggregation by 59+/-14% (50 mg [mean+/-SD]; n=8), 90+/-12% (100 mg), and 99+/-2% (150 mg) 8 hours after administration. Correlations between activity and Fradafiban plasma levels were identical after Fradafiban and Lefradafiban treatment. After day 1, oral TID Lefradafiban treatment for 7 days inhibited aggregation by > or = 31+/-9.6% (25 mg TID; n=8), 53+/-12% (50 mg; n=7), and 88+/-6.6% (75 mg; n=8) just before the next dose. A similar correlation between the activity and Fradafiban plasma levels was observed at days 1, 2, and 7.
Oral administration of Lefradafiban maintains the potent platelet GP IIb/IIIa antagonism of Fradafiban during treatment of healthy subjects for 1 week without signs of loss of the antiplatelet activity.
临床试验已证明血小板糖蛋白(GP)IIb/IIIa拮抗剂能有效预防急性血栓形成事件。口服活性GP IIb/IIIa拮抗剂对于评估长期治疗的临床益处至关重要。因此,我们在健康受试者中研究了GP IIb/IIIa拮抗剂弗拉达非班(BIBU 52;弗拉达非班是BIBU 52的推荐国际非专利名称)及其口服前体药物左拉达非班(BIBU 104;左拉达非班是BIBU 104的推荐国际非专利名称)对血小板的抑制作用。
在130名健康男性受试者中进行了双盲、安慰剂对照研究,评估了弗拉达非班和左拉达非班的活性及血浆水平。在30分钟内持续输注1至15毫克弗拉达非班可在体外对富含血小板血浆中20微摩尔/升二磷酸腺苷(ADP)(5毫克,给药后27分钟时100%抑制)以及1.0(5毫克,100%)和10微克/毫升(15毫克,97±3%)胶原诱导的血小板聚集产生可逆性抑制。单次口服左拉达非班剂量在给药8小时后对ADP诱导的聚集抑制率分别为59±14%(50毫克[均值±标准差];n = 8)、90±12%(100毫克)和99±2%(150毫克)。弗拉达非班和左拉达非班治疗后活性与弗拉达非班血浆水平之间的相关性相同。第1天后,口服左拉达非班每日三次,连续7天,在下一次给药前对聚集的抑制率分别为≥31±9.6%(25毫克每日三次;n = 8)、53±12%(50毫克;n = 7)和88±6.6%(75毫克;n = 8)。在第1、2和7天观察到活性与弗拉达非班血浆水平之间存在类似的相关性。
在健康受试者治疗1周期间,口服左拉达非班可维持弗拉达非班对血小板GP IIb/IIIa的强效拮抗作用,且无抗血小板活性丧失的迹象。
