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组织型纤溶酶原激活剂与噻氯匹定联合治疗兔急性血栓栓塞性中风模型

Combination tissue plasminogen activator and ticlopidine therapy in a rabbit model of acute thromboembolic stroke.

作者信息

Bednar M M, Raymond-Russell S J, Booth C L, Gross C E

机构信息

Division of Neurosurgery, University of Vermont, Burlington, USA.

出版信息

Neurol Res. 1996 Feb;18(1):45-8. doi: 10.1080/01616412.1996.11740376.

DOI:10.1080/01616412.1996.11740376
PMID:8714536
Abstract

The successful application of thrombolytic therapy to acute myocardial infarction has prompted a reinvestigation of thrombolytic therapy for acute stroke. However, an examination of safety and efficacy of thrombolytic therapy in acute thromboembolic stroke has precluded the entry of patients taking either antiplatelet or anticoagulant therapy. It was therefore of interest, in an established rabbit model of thromboembolic stroke, to examine the use of tissue plasminogen activator therapy in combination with ticlopidine treatment. Following ticlopidine administration (10 mg kg-1, i.v., daily for 5 days), rabbits (n = 7) were embolized by injecting a tin-laden clot into the internal carotid artery with clot placement confirmed by x-ray. Three hours later, t-PA was initiated as a square-wave pulse (6.3 mg kg-1 total dose, given as a 20% bolus, with the remainder administered over 2 h as a continuous infusion). The protocol was continued for a total of 7 h following embolization. Complete clot lysis was demonstrated in 6 of 7 animals. Brain infarct size (triphenyltetrazolium chloride staining) was 36.0 +/- 12.9% hemisphere (mean +/- SEM). Both clot lysis rate and infarct size were very similar to that previously seen following administration of t-PA alone (58% and 31.6 +/- 6.4% hemisphere, respectively) but in marked contrast to previous results seen with intravenous aspirin (no clot lysis). These results suggest that antiplatelet agents used clinically for stroke prophylaxis (aspirin or ticlopidine) may influence the success rate of thrombolysis following initiation of thrombolytic therapy for acute thromboembolic stroke.

摘要

溶栓疗法在急性心肌梗死中的成功应用促使人们对急性中风的溶栓疗法重新进行研究。然而,对急性血栓栓塞性中风溶栓疗法安全性和有效性的研究排除了正在接受抗血小板或抗凝治疗的患者入组。因此,在已建立的血栓栓塞性中风兔模型中,研究组织型纤溶酶原激活剂疗法与噻氯匹定联合使用的情况就很有意义。在给予噻氯匹定(10毫克/千克,静脉注射,每日1次,共5天)后,通过向颈内动脉注射含锡凝块对兔(n = 7)进行栓塞,通过X射线确认凝块位置。3小时后,开始给予t-PA,呈方波脉冲给药(总剂量6.3毫克/千克,先给予20%的推注剂量,其余剂量在2小时内持续输注)。栓塞后该方案共持续7小时。7只动物中有6只实现了凝块完全溶解。脑梗死面积(用氯化三苯基四氮唑染色)为半球的36.0±12.9%(平均值±标准误)。凝块溶解率和梗死面积与之前单独给予t-PA后的情况非常相似(分别为58%和半球的31.6±6.4%),但与静脉注射阿司匹林的先前结果(无凝块溶解)形成显著对比。这些结果表明,临床上用于预防中风的抗血小板药物(阿司匹林或噻氯匹定)可能会影响急性血栓栓塞性中风溶栓治疗开始后的溶栓成功率。

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