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经PEDF治疗的缺血性大鼠脊髓中与神经可塑性相关分子的行为改善及调节

Behavioral improvement and regulation of molecules related to neuroplasticity in ischemic rat spinal cord treated with PEDF.

作者信息

Batista Chary Marquez, Bianqui Leonardo Luis Torres, Zanon Bruno Bonganha, Ivo Mauricio Menezes Aben Athar, Oliveira Gabriela Pintar de, Maximino Jessica Ruivo, Chadi Gerson

机构信息

Neuroregeneration Center, Department of Neurology, School of Medicine, University of São Paulo, Avenida Dr. Arnaldo 455, 2nd Floor, Room 2119, 01246-903-São Paulo, SP, Brazil.

出版信息

Neural Plast. 2014;2014:451639. doi: 10.1155/2014/451639. Epub 2014 Jul 3.

Abstract

Pigment epithelium derived factor (PEDF) exerts trophic actions to motoneurons and modulates nonneuronal restorative events, but its effects on neuroplasticity responses after spinal cord (SC) injury are unknown. Rats received a low thoracic SC photothrombotic ischemia and local injection of PEDF and were evaluated behaviorally six weeks later. PEDF actions were detailed in SC ventral horn (motor) in the levels of the lumbar central pattern generator (CPG), far from the injury site. Molecules related to neuroplasticity (MAP-2), those that are able to modulate such event, for instance, neurotrophic factors (NT-3, GDNF, BDNF, and FGF-2), chondroitin sulfate proteoglycans (CSPG), and those associated with angiogenesis and antiapoptosis (laminin and Bcl-2) and Eph (receptor)/ephrin system were evaluated at cellular or molecular levels. PEDF injection improved motor behavioral performance and increased MAP-2 levels and dendritic processes in the region of lumbar CPG. Treatment also elevated GDNF and decreased NT-3, laminin, and CSPG. Injury elevated EphA4 and ephrin-B1 levels, and PEDF treatment increased ephrin A2 and ephrins B1, B2, and B3. Eph receptors and ephrins were found in specific populations of neurons and astrocytes. PEDF treatment to SC injury triggered neuroplasticity in lumbar CPG and regulation of neurotrophic factors, extracellular matrix molecules, and ephrins.

摘要

色素上皮衍生因子(PEDF)对运动神经元发挥营养作用并调节非神经元修复事件,但其对脊髓(SC)损伤后神经可塑性反应的影响尚不清楚。大鼠接受低位胸段脊髓光血栓性缺血并局部注射PEDF,六周后进行行为评估。在远离损伤部位的腰髓中央模式发生器(CPG)水平的脊髓腹角(运动)中详细研究了PEDF的作用。在细胞或分子水平上评估了与神经可塑性相关的分子(MAP-2)、能够调节此类事件的分子,例如神经营养因子(NT-3、GDNF、BDNF和FGF-2)、硫酸软骨素蛋白聚糖(CSPG)以及与血管生成和抗凋亡相关的分子(层粘连蛋白和Bcl-2)和Eph(受体)/ephrin系统。注射PEDF改善了运动行为表现,并增加了腰髓CPG区域的MAP-2水平和树突状突起。治疗还提高了GDNF水平并降低了NT-3、层粘连蛋白和CSPG水平。损伤使EphA4和ephrin-B1水平升高,而PEDF治疗增加了ephrin A2以及ephrin B1、B2和B3的水平。在特定的神经元和星形胶质细胞群体中发现了Eph受体和ephrin。对脊髓损伤进行PEDF治疗可引发腰髓CPG的神经可塑性以及神经营养因子、细胞外基质分子和ephrin的调节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f3b2/4106224/b397cca3ba4b/NP2014-451639.001.jpg

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