Weinheimer C J, James H L, Kalyan N K, Wilhelm J, Lee S G, Hung P P, Sobel B E, Bergmann S R
Cardiovascular Division, Washington University School of Medicine, St. Louis, Mo 63110.
Circulation. 1991 Apr;83(4):1429-36. doi: 10.1161/01.cir.83.4.1429.
Despite the utility of tissue-type plasminogen activator (t-PA) in eliciting coronary thrombolysis clinically, early reocclusion remains a problem, occurring despite anticoagulation in 5-30% of patients with initially successful recanalization. This study evaluated the utility of Hybrid-B, a molecular variant of t-PA with a prolonged half-life in the circulation, in eliciting coronary thrombolysis and maintaining patency in the presence of a continuing thrombogenic stimulus.
In intact, anesthetized dogs, either 18 mg Hybrid-B over 30 minutes (n = 15) or 50 mg t-PA (Activase) over 60 minutes (n = 8) was administered starting 60 minutes after left anterior descending coronary artery occlusion was induced with a thrombogenic copper coil. Time to lysis averaged 54 +/- 26 (means +/- SD) minutes and 64 +/- 34 minutes with Hybrid-B and t-PA, respectively (p = NS). When Hybrid-B was administered as a bolus (20 mg over 1 minute) to induce a high initial concentration in blood, time to lysis was shortened markedly and averaged 15 +/- 5 minutes. Dogs given Hybrid-B by either infusion or bolus exhibited prolonged time to reocclusion (337 +/- 192 minutes compared with 192 +/- 125 minutes in dogs given t-PA, p less than 0.03), reflecting maintenance of a subthrombolytic but persistently active concentration of activator in blood. Despite the persistence of Hybrid-B in blood, concentrations of fibrinogen and alpha 2-antiplasmin were not depleted markedly and remained at 77 +/- 25 and 56 +/- 24%, respectively, of control values.
Thus, Hybrid-B, a novel variant of t-PA with unique pharmacokinetic properties, elicits prompt, sustained, and clot-selective coronary thrombolysis.
尽管组织型纤溶酶原激活剂(t-PA)在临床上用于引发冠状动脉溶栓具有实用性,但早期再闭塞仍是一个问题,在最初成功再通的患者中,尽管进行了抗凝治疗,仍有5%-30%的患者会出现再闭塞。本研究评估了Hybrid-B(一种在循环中半衰期延长的t-PA分子变体)在引发冠状动脉溶栓以及在存在持续血栓形成刺激的情况下维持血管通畅方面的效用。
在完整的麻醉犬中,自使用致血栓形成的铜线圈诱导左前降支冠状动脉闭塞60分钟后开始给药,分别以30分钟内给予18mg Hybrid-B(n = 15)或60分钟内给予50mg t-PA(阿替普酶)(n = 8)。Hybrid-B组和t-PA组的溶栓时间平均分别为54±26(均值±标准差)分钟和64±34分钟(p = 无显著性差异)。当以推注方式(1分钟内给予20mg)给予Hybrid-B以在血液中诱导高初始浓度时,溶栓时间明显缩短,平均为15±5分钟。通过输注或推注给予Hybrid-B的犬再闭塞时间延长(分别为337±192分钟,而给予t-PA的犬为192±125分钟,p<0.03),这反映出血液中维持了亚溶栓但持续有活性的激活剂浓度。尽管Hybrid-B在血液中持续存在,但纤维蛋白原和α₂-抗纤溶酶的浓度并未明显降低,分别维持在对照值的77±25%和56±24%。
因此,Hybrid-B作为一种具有独特药代动力学特性的新型t-PA变体,可引发迅速、持续且具有凝块选择性的冠状动脉溶栓。
