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重组组织型纤溶酶原激活剂(rt-PA)对大型动物脑出血模型中水肿形成的长期影响。

The long-term effect of recombinant tissue-plasminogen-activator (rt-PA) on edema formation in a large-animal model of intracerebral hemorrhage.

作者信息

Thiex Ruth, Küker Wilhelm, Müller Harald D, Rohde Ina, Schröder J Michael, Gilsbach Joachim M, Rohde Veit

机构信息

Department of Neurosurgery, Aachen University, Pauwelsstr. 30, 52057 Aachen, Germany.

出版信息

Neurol Res. 2003 Apr;25(3):254-62. doi: 10.1179/016164103101201463.

Abstract

Hematoma puncture, fibrinolysis, and aspiration of the liquefied clot is a promising new treatment strategy for large intracerebral hemorrhages (ICH). Characteristics of the cellular injury and neuronal and glial cell death associated with ICH and the administration of fibrinolytic agents still need to be defined. We developed a porcine model to study the histopathological effects of recombinant tissue-Plasminogen-Activator (rt-PA) on perihematomatous cell integrity. In 20 pigs, lobar hematomas were induced by intracranial pressure (ICP)-controlled injections of 7.6 +/- 1.6 ml of autologous blood into the white matter of the right frontal hemisphere. In nine animals, the clots were lysed with rt-PA, thereby facilitating aspiration 2 h after hematoma induction. In 11 control pigs, the hematoma resorption followed its natural course. The rate of hematoma reduction and edema formation over 10 days was evaluated on planimetry of the MRI data and correlated to the histopathological changes found at autopsy. Although rt-PA significantly accelerated clot resolution compared to controls (p < 0.02), the increase of perihematomatous edema volume within 10 days was not significantly ameliorated in rt-PA-treated animals compared to controls on MRI. The extent of inflammatory infiltrates on histology was more pronounced in animals treated with rt-PA. In conclusion, despite significant reduction in the size of the hematoma clot liquefication with rt-PA and aspiration invokes a substantial inflammatory response when studied after 10 days and does not result in a reduction of the perihematomatous edema.

摘要

血肿穿刺、纤维蛋白溶解及抽吸液化血凝块是治疗大面积脑出血(ICH)的一种有前景的新策略。与脑出血及纤维蛋白溶解剂给药相关的细胞损伤以及神经元和胶质细胞死亡的特征仍有待明确。我们建立了一个猪模型来研究重组组织型纤溶酶原激活剂(rt-PA)对血肿周围细胞完整性的组织病理学影响。在20头猪中,通过在右额叶白质内以颅内压(ICP)控制注射7.6±1.6 ml自体血诱导叶性血肿。在9只动物中,用rt-PA溶解血凝块,从而在血肿诱导后2小时便于抽吸。在11只对照猪中,血肿吸收遵循其自然进程。通过对MRI数据进行平面测量评估10天内血肿缩小率和水肿形成情况,并将其与尸检时发现的组织病理学变化相关联。尽管与对照组相比,rt-PA显著加速了血凝块溶解(p<0.02),但在MRI上,与对照组相比,rt-PA治疗的动物在10天内血肿周围水肿体积的增加并未得到显著改善。rt-PA治疗的动物组织学上炎症浸润程度更明显。总之,尽管rt-PA使血肿凝块液化大小显著减小,且抽吸在10天后研究时引发了大量炎症反应,但并未导致血肿周围水肿减轻。

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