实验性栓塞性脑卒中的溶栓治疗。

K Overgaard
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引用次数: 0

摘要

溶栓治疗在急性心肌梗死中的作用已被充分证实。在急性脑梗死中,溶栓治疗已经在小系列患者中进行了评估。溶栓治疗的目的是通过快速动脉再通来避免或减少神经元组织的缺血性损伤。在脑血管闭塞的溶栓治疗中,再灌注的病理生理需要进一步研究和记录。这篇综述描述了栓塞性中风的溶栓研究,用动物在颈动脉内注射血凝块栓塞。血管造影和脑血流量测量证实血管闭塞。重组组织型纤溶酶原激活剂在不同时间后开始溶栓治疗。血管造影及临床病理解剖检查再灌注、细胞功能、脑损伤情况。我们主要根据自己的研究结果,对缺血性脑卒中提出了以下结论:(a)动脉闭塞所致脑梗死是由于再灌注延迟、不完全或无再灌注所致。痉挛,或血液动力学机制,似乎只是次要的。(b)动物模型早期溶栓治疗可增加再灌注程度,减少脑损伤、临床缺陷和死亡率。(c)早期动脉再灌注减少脑梗死及相关水肿。在早期再灌注时,脑损伤的程度与缺血发生的延迟时间有关。(d)脑昏迷是由动脉闭塞引起的,随后是非常早期的自发或诱导的再灌注,因为神经元暂时失去功能而没有死亡。(e)实验性中风中的多个栓塞性微凝块比单个大凝块造成更大的脑损伤,而对于血栓,脑损伤的程度取决于栓塞的结构组成和体积。(f)实验性栓塞性中风的再通能力与栓子中红细胞的数量有关,与栓子的体积、纤维蛋白含量和凝块密度成反比。(g)实验性脑卒中的梗死限制作用可通过缺血性神经保护剂或单独或与溶栓治疗联合使用的低温获得,从而进一步减少脑损伤。
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Thrombolytic therapy in experimental embolic stroke.

The effect of thrombolytic therapy is well-documented in acute myocardial infarction. In acute cerebral infarction, thrombolytic therapy has been evaluated in small series of patients. The point of thrombolytic therapy is to avoid or reduce ischemic damage of neuronal tissue by rapid arterial recanalization. In thrombolytic therapy of cerebral vascular occlusion, the pathophysiology of reperfusion needs further investigation and documentation. This review describes studies of thrombolysis in embolic stroke using animals embolized by intracarotid injections of blood clots. Vascular occlusion was demonstrated by angiography and measurement of cerebral blood flow. Thrombolytic therapy with recombinant tissue-type plasminogen activator was initiated after varying periods of time. Reperfusion, cellular function, and brain damage were examined by angiography and by clinical and pathoanatomical examination. Based mainly on results from our own investigations, the following theses concerning ischemic stroke were made: (a) Cerebral infarction caused by arterial occlusion is due to delayed, incomplete, or no reperfusion. Spasms, or hemodynamic mechanisms, seem to be of only minor importance. (b) Early thrombolytic therapy in animal models increases the degree of reperfusion and reduces brain damage, clinical deficits, and mortality. (c) Early arterial reperfusion reduces cerebral infarction and related edema. With early reperfusion, the extent of brain damage correlates to the length of the delay from onset of ischemia. (d) Cerebral stunning is caused by arterial occlusion followed by very early spontaneous or induced reperfusion, as neurons temporarily lose their functional capabilities without dying. (e) Multiple embolic microclots in experimental stroke result in more brain damage than a single macroclot, and with clots the extent of brain damage is dependent on the structural composition and volume of emboli. (f) The ability to recanalization in experimental embolic stroke is related to the amount of red cells in the emboli and inversely related to the volume of emboli and to the fibrin content and density of the clots. (g) Infarct-limiting effects in experimental stroke can be obtained by ischemic neuroprotectants or by hypothermia, either alone or with thrombolytic therapy, which then reduces brain damage further.

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