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Post-acute delivery of erythropoietin induces stroke recovery by promoting perilesional tissue remodelling and contralesional pyramidal tract plasticity

机译:促红细胞生成素的急性后递送通过促进病灶周围组织重塑和对位锥体束可塑性来诱导中风恢复

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摘要

The promotion of post-ischaemic motor recovery remains a major challenge in clinical neurology. Recently, plasticity-promoting effects have been described for the growth factor erythropoietin in animal models of neurodegenerative diseases. To elucidate erythropoietin's effects in the post-acute ischaemic brain, we examined how this growth factor influences functional neurological recovery, perilesional tissue remodelling and axonal sprouting of the corticorubral and corticobulbar tracts, when administered intra-cerebroventricularly starting 3 days after 30 min of middle cerebral artery occlusion. Erythropoietin administered at 10 IU/day (but not at 1 IU/day), increased grip strength of the contralesional paretic forelimb and improved motor coordination without influencing spontaneous locomotor activity and exploration behaviour. Neurological recovery by erythropoietin was associated with structural remodelling of ischaemic brain tissue, reflected by enhanced neuronal survival, increased angiogenesis and decreased reactive astrogliosis that resulted in reduced scar formation. Enhanced axonal sprouting from the ipsilesional pyramidal tract into the brainstem was observed in vehicle-treated ischaemic compared with non-ischaemic animals, as shown by injection of dextran amines into both motor cortices. Despite successful remodelling of the perilesional tissue, erythropoietin enhanced axonal sprouting of the contralesional, but not ipsilesional pyramidal tract at the level of the red and facial nuclei. Moreover, molecular biological and histochemical studies revealed broad anti-inflammatory effects of erythropoietin in both hemispheres together with expression changes of plasticity-related molecules that facilitated contralesional axonal growth. Our study establishes a plasticity-promoting effect of erythropoietin after stroke, indicating that erythropoietin acts via recruitment of contralesional rather than of ipsilesional pyramidal tract projections
机译:促进缺血后运动恢复仍然是临床神经病学的主要挑战。最近,已经描述了在神经退行性疾病的动物模型中促生长因子促红细胞生成素的可塑性促进作用。为了阐明促红细胞生成素在急性缺血后脑中的作用,我们研究了在大脑中部中部30分钟后3天开始在脑室内施用时,该生长因子如何影响功能性神经系统恢复,皮损和皮层皮层的轴突发芽。动脉闭塞。促红细胞生成素以10 IU /天(但不是1 IU /天)给药,增加了对侧阵发性前肢的握力,并改善了运动协调性,而不会影响自发运动能力和探索行为。促红细胞生成素的神经功能恢复与缺血性脑组织的结构重塑有关,表现为神经元存活率提高,血管生成增加和反应性星形胶质增生减少,从而减少了疤痕的形成。与非局部缺血的动物相比,在媒介物处理的局部缺血中观察到了从同侧锥体束到脑干的轴突发芽增强,这是通过向两个运动皮层注射右旋糖酐胺显示的。尽管成功地重建了病灶周围组织,但促红细胞生成素在红色和面核水平上增强了对病灶的轴突发芽,但未增强同病灶的锥体束。此外,分子生物学和组织化学研究显示,促红细胞生成素在两个半球均具有广泛的抗炎作用,并且可塑性相关分子的表达发生变化,促进对侧轴突生长。我们的研究建立了促红细胞生成素在中风后的可塑性促进作用,表明促红细胞生成素是通过募集对侧的而不是同侧的锥体束投影来起作用的

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