体外和体内联合评估新型口服抗凝剂加重实验性脑出血的程度。

Juliana R P Ferreira, Isabela D Sucupira, Gabriella M C Carvalho, Fernando F Paiva, Pedro M Pimentel-Coelho, Paulo H Rosado-de-Castro, Paulo A S Mourão, Roberto J C Fonseca
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引用次数: 0

摘要

脑出血是抗凝治疗最严重的并发症,但不同类型的口服抗凝剂对脑出血扩张的影响尚不清楚。临床研究揭示了有争议的结果;需要更可靠和长期的临床评估来确定其结果。另一种方法是在动物脑出血的实验模型中测试这些药物的效果。目的观察新型口服抗凝剂达比加群酯、利伐沙班和阿哌沙班在纹状体注射胶原酶致脑出血大鼠实验模型中的作用。采用华法林进行比较。方法采用体外抗凝血试验和静脉血栓形成实验模型,确定抗凝血药物达到最大作用所需的剂量和时间。随后,使用相同的参数评估抗凝剂给药后的脑血肿体积。通过磁共振成像、苏木精和伊红染色、Evans蓝外渗评估脑血肿体积。神经运动功能通过升高体摆动试验评估。结果与结论与对照组相比,新型口服抗凝剂未增加颅内出血,而华法林明显促进血肿扩张,磁共振成像和H&E染色显示。达比加群酯引起埃文斯蓝色外渗的轻微但有统计学意义的增加。我们没有观察到实验组之间在高摆体测试中的显著差异。新的口服抗凝剂可能比华法林更好地控制脑出血。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A Combination of Ex Vivo and In Vivo Strategies for Evaluating How Much New Oral Anticoagulants Exacerbate Experimental Intracerebral Bleeding.

A Combination of Ex Vivo and In Vivo Strategies for Evaluating How Much New Oral Anticoagulants Exacerbate Experimental Intracerebral Bleeding.

A Combination of Ex Vivo and In Vivo Strategies for Evaluating How Much New Oral Anticoagulants Exacerbate Experimental Intracerebral Bleeding.

A Combination of Ex Vivo and In Vivo Strategies for Evaluating How Much New Oral Anticoagulants Exacerbate Experimental Intracerebral Bleeding.

Background  Intracerebral hemorrhage is the most serious complication of anticoagulant therapy but the effects of different types of oral anticoagulants on the expansion of these hemorrhages are still unclear. Clinical studies have revealed controversial results; more robust and long-term clinical evaluations are necessary to define their outcomes. An alternative is to test the effect of these drugs in experimental models of intracerebral bleeding induced in animals. Aims  To test new oral anticoagulants (dabigatran etexilate, rivaroxaban, and apixaban) in an experimental model of intracerebral hemorrhage induced by collagenase injection into the brain striatum of rats. Warfarin was used for comparison. Methods  Ex vivo anticoagulant assays and an experimental model of venous thrombosis were employed to determine the doses and periods of time required for the anticoagulants to achieve their maximum effects. Subsequently, volumes of brain hematoma were evaluated after administration of the anticoagulants, using these same parameters. Volumes of brain hematoma were evaluated by magnetic resonance imaging, H&E (hematoxylin and eosin) staining, and Evans blue extravasation. Neuromotor function was assessed by the elevated body swing test. Results and Conclusions  The new oral anticoagulants did not increase intracranial bleeding compared with control animals, while warfarin markedly favored expansion of the hematomas, as revealed by magnetic resonance imaging and H&E staining. Dabigatran etexilate caused a modest but statistically significant increase in Evans blue extravasation. We did not observe significant differences in elevated body swing tests among the experimental groups. The new oral anticoagulants may provide a better control over a brain hemorrhage than warfarin.

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