Michael E. DeBakey VA Medical Center Stroke Program and Department of Neurology, Baylor College of Medicine, 2002 Holcombe Blvd (127), Houston, TX, 77030, USA,
Transl Stroke Res. 2010 Sep;1(3):170-7. doi: 10.1007/s12975-010-0026-4.
Thrombolysis remains a mainstay in the treatment of ischemic stroke. While not usually considered in the spectrum of clot lysis, experimental data show that inhibition of the platelet glycoprotein (GP) IIb/IIIa receptor can reduce as well as reverse thrombus formation and improve microvascular flow in stroke models. However, a recent clinical trial of GP IIb/IIIa inhibition in stroke did not demonstrate clinical benefit and was associated with increased hemorrhage. Based on an understanding of the relationship between GP IIb/IIIa receptor inhibition, efficacy and hemorrhage, we hypothesized that a lower dose of abciximab would achieve a favorable range of platelet inhibition and potentially good clinical outcomes. Forty-four patients with suspected large vessel occlusion, who were not eligible for rt-PA were offered treatment with approximately 30% lower total dose of intravenous abciximab if within 6 h for anterior circulation or 24 h for posterior circulation stroke (later modified to 12 h). Concomitant anticoagulation, usually with unfractionated heparin was employed. The extent of platelet inhibition was measured in 21 patients. Hemorrhage rate and 90-day functional outcomes and mortality were obtained. A matching algorithm involving finding the nearest neighbor from individual subjects in the control arm of the NINDS rt-PA database was used to compare outcomes at similar baseline characteristics and gender. Mean platelet inhibition was 92.1 ± 6.7% vs inhibition reported with percutaneous coronary intervention (PCI) of 96 ± 10; p = 0.08. Successful matching to NINDS controls was accomplished: after outlier elimination, median and mean NIHSS of the abciximab subjects compared to NINDS controls was 16.5 vs 15.5 (p = 0.92) and 16.3 vs 16.0 (p = 0.86). Mean age was 67.2 vs 67.1 (p = 0.97). Mean glucose was 141 vs 142 (p = 0.92). There was one symptomatic hemorrhage; minor hemorrhages occurred in 9%. The percent of patients who achieved an mRS 0-2 or died in the treated vs matched NINDS control patients was 63 vs 38 (p = .02) and 23 vs 23 (p = 1.0). Our pilot results indicated that a lower dose of abciximab results in platelet inhibition similar to that achieved in the coronary vascular bed during PCI. Comparison to matched historical controls suggests that this lower dose in combination therapy may be safe and effective therapy for thrombotic stroke and a randomized trial is warranted.
溶栓仍然是治疗缺血性脑卒中的主要方法。虽然通常不考虑在血栓溶解的范围内,但实验数据表明,抑制血小板糖蛋白(GP)IIb/IIIa 受体可以减少血栓形成并改善中风模型中的微血管血流。然而,最近一项关于中风中 GP IIb/IIIa 抑制的临床试验并未显示出临床益处,并且与出血增加有关。基于对 GP IIb/IIIa 受体抑制、疗效和出血之间关系的理解,我们假设较低剂量的阿昔单抗可以达到理想的血小板抑制范围,并可能获得良好的临床结果。44 名疑似大血管闭塞的患者不符合 rt-PA 治疗条件,如果在前循环 6 小时内或后循环 24 小时内(后来修改为 12 小时内)接受治疗,将给予约 30%的静脉内阿昔单抗总剂量。同时使用普通肝素进行抗凝治疗。在 21 名患者中测量了血小板抑制程度。获得了出血率和 90 天的功能结局和死亡率。使用涉及在 NINDS rt-PA 数据库的对照组中找到每个个体对象的最近邻的匹配算法来比较具有相似基线特征和性别的结果。平均血小板抑制率为 92.1±6.7%,与经皮冠状动脉介入治疗(PCI)的 96±10%相比;p=0.08。成功地与 NINDS 对照组进行了匹配:消除离群值后,与 NINDS 对照组相比,阿昔单抗组的中位数和平均 NIHSS 为 16.5 与 15.5(p=0.92)和 16.3 与 16.0(p=0.86)。平均年龄为 67.2 与 67.1(p=0.97)。平均血糖为 141 与 142(p=0.92)。有一例症状性出血;9%发生轻微出血。治疗组与匹配的 NINDS 对照组患者中达到 mRS 0-2 或死亡的患者比例为 63%与 38%(p=0.02)和 23%与 23%(p=1.0)。我们的初步结果表明,较低剂量的阿昔单抗可达到与 PCI 期间在冠状动脉血管床中相似的血小板抑制。与匹配的历史对照相比,这种低剂量联合治疗可能是血栓性中风的安全有效治疗方法,需要进行随机试验。
