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Dose Effect Evaluation and Therapeutic Window of the Neuro-EPO Nasal Application for the Treatment of the Focal Ischemia Model in the Mongolian Gerbil

机译:神经-EPO鼻剂治疗蒙古沙鼠局灶性缺血模型的剂量效果评估和治疗窗口

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摘要

Cerebrovascular disease is the third leading cause of death and the leading cause of disability in Cuba and in several developed countries. A possible neuroprotective agent is the rHu-EPO, whose effects have been demonstrated in models of brain ischemia. The Neuro-EPO is a derivative of the rHu-EPO that avoids the stimulation of erythropoiesis. The aim of this study was to determine the Neuro-EPO delivery into the central nervous system (CNS) to exert a neuroprotective effect in cerebral ischemia model of the Mongolian gerbil. The Neuro-EPO in a rate of 249.4 UI every 8 hours for 4 days showed 25% higher viability efficacy (P > 0.01), improving neurological score and behavior of the spontaneous exploratory activity, the preservation of CA3 areas of the hippocampus, the cortex, and thalamic nuclei in the focal ischemia model of the Mongolian gerbil. In summary, this study, the average dose-used Neuro-EPO (249.4 UI/10 μL/every 8 hours for 4 days), proved to be valid indicators of viability, neurological status, and spontaneous exploratory activity, being significantly lower than that reported for the systemically use of the rHu-EPO as a neuroprotectant. Indeed, up to 12 h after brain ischemia is very positive Neuro-EPO administration by the nasal route as a candidate for neuroprotection.
机译:在古巴和一些发达国家,脑血管疾病是第三大死亡原因和致残因素。可能的神经保护剂是rHu-EPO,其作用已在脑缺血模型中得到证实。 Neuro-EPO是rHu-EPO的衍生物,可避免刺激红细胞生成。这项研究的目的是确定神经-EPO传递到中枢神经系统(CNS),以在蒙古沙鼠的脑缺血模型中发挥神经保护作用。 Neuro EPO以每8小时249.4 24UI的速率持续4天,表现出25%的生存力提高(P> 0.01),改善了神经系统评分和自发探索活动的行为,保护了海马,皮层的CA3区域和蒙古沙鼠的局灶性缺血模型中的丘脑核。总而言之,这项研究表明,平均剂量使用的Neuro-EPO(249.4 UI /10μL/每8小时,每4小时一次)可作为生存能力,神经系统状态和自发探索活动的有效指标,远低于该指标。报道了rHu-EPO作为神经保护剂的全身使用。确实,在脑缺血后长达12小时,通过鼻腔途径给予Neuro-EPO非常积极,可以作为神经保护的候选药物。

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