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首页> 外文期刊>Neurological Research: An Interdisciplinary Quarterly Journal >Therapeutic time window of hypothermia is broader than cerebral artery flushing in carotid saline infusion after transient focal ischemic stroke in rats
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Therapeutic time window of hypothermia is broader than cerebral artery flushing in carotid saline infusion after transient focal ischemic stroke in rats

机译:在短暂性局灶性缺血性脑卒中后,低温治疗的治疗时间范围比颈动脉盐水注入中的脑动脉冲洗更宽

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Object: Intracarotid cold saline infusion (ICSI) protects against ischemic stroke not only due to the resulting hypothermia, but also as a result of the cerebral artery flushing. To assess the relative benefit of hypothermia and cerebral artery flushing in neuroprotection, hypothermic and normothermic saline infusions were administrated over a serial time points after the initiation of reperfusion in a rat ischemia model. Methods: Ischemic strokes were induced in Sprague-Dawley rats (n5115) by occluding the middle cerebral artery for 2 hours using an intraluminal filament. In the hypothermic groups, the brain temperature was lowered to 33-34°C for 20 minutes by ICSI at three time points (0, 1, and 2 hours) after reperfusion. Correspondingly, in the normothermic groups, the brain temperature was maintained at normal levels during intracarotid normothermic saline infusion (INSI) for 20 minutes at the same time points. After 48-hour reperfusion, infarct sizes and brain water contents were determined using 2,3,5-triphenyltetrazolium chloride (TTC) staining and the dry-wet weight method, respectively. Levels of neuron-specific enolase (NSE), S100beta, and matrix metalloproteinase 9 (MMP9) in the serum were measured by enzyme-linked immunoassay (ELISA). Neurological deficits were also evaluated. Results: Immediate infusion after the onset of reperfusion (0 hour) did not result in significant difference for reductions of infarct sizes, neurological deficits or S100beta serum levels between ICSI and INSI groups, compared with the non-infusion group. However, brain water content and NSE serum level were significantly lower in the ICSI group than the non-infusion group. When the infusions were started 1 hour after reperfusion, both ICSI and INSI infusions still reduced the infarct sizes, but only ICSI significantly decreased the brain water content, neurological deficits and S100beta serum level. All therapeutic effects of INSI disappeared when infusions were started 2 hours after reperfusion, whereas infarct size, neurological deficits and S100beta serum level were still reduced significantly in ICSI group, compared with the non-infusion group. Conclusions: The neuroprotection of hypothermia and cerebral artery flushing induced by selective carotid infusion after ischemia weakens as the length of time between the reperfusion and infusion increases. The therapeutic time window of brain hypothermia induced by cold saline infusion is broader than cerebral artery flushing induced by normothermic saline infusion.
机译:目的:颈动脉冷盐水输注(ICSI)不仅可以防止因体温过低引起的缺血性中风,而且还可以防止因脑动脉潮红而引起的缺血性中风。为了评估低温和脑动脉潮红对神经保护的相对益处,在大鼠局部缺血模型中,在开始再灌注后的连续时间点内,给予低温和常温生理盐水输注。方法:通过使用腔内灯丝阻塞大脑中动脉2小时,在Sprague-Dawley大鼠(n5115)中诱发缺血性中风。在低温组中,ICSI在再灌注后的三个时间点(0、1、2小时)将脑温降低至33-34°C,持续20分钟。相应地,在常温组中,在同一时间点的颈内常温生理盐水输注(INSI)20分钟期间,脑温保持在正常水平。再灌注48小时后,分别使用2,3,5-三苯基四唑氯化物(TTC)染色和干湿重法测定梗塞面积和脑含水量。血清中神经元特异性烯醇化酶(NSE),S100beta和基质金属蛋白酶9(MMP9)的水平通过酶联免疫法(ELISA)测定。还评估了神经功能缺损。结果:与非输注组相比,ICSI组和INSI组之间在再灌注开始后(0小时)立即输注并没有导致梗死面积,神经功能缺损或S100beta血清水平降低的显着差异。但是,ICSI组的脑含水量和NSE血清水平明显低于非输注组。当再灌注后1小时开始输注时,ICSI和INSI输注仍会减小梗塞面积,但只有ICSI才能显着降低脑含水量,神经功能缺损和S100beta血清水平。再灌注后2小时开始输注时,INSI的所有治疗作用均消失,而与非输注组相比,ICSI组的梗死面积,神经功能缺损和S100beta血清水平仍显着降低。结论:随着再灌注和灌注时间的延长,局部缺血后选择性颈动脉灌注对体温过低和脑动脉潮红的神经保护作用减弱。冷盐水注入引起的脑低温的治疗时间窗比普通生理盐水注入引起的脑动脉潮红更宽。

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