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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Vascular endothelial growth factor improves functional outcome and decreases secondary degeneration in experimental spinal cord contusion injury.
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Vascular endothelial growth factor improves functional outcome and decreases secondary degeneration in experimental spinal cord contusion injury.

机译:血管内皮生长因子改善了功能结果并减少了实验性脊髓挫伤中的继发性变性。

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摘要

Spinal cord injury leads to acute local ischemia, which may contribute to secondary degeneration. Hypoxia stimulates angiogenesis through a cascade of events, involving angiogenesis stimulatory substances, such as vascular endothelial growth factor (VEGF). To test the importance of angiogenesis for functional outcome and wound healing in spinal cord injury VEGF165 (proangiogenic), Ringer's (control) or angiostatin (antiangiogenic) were delivered locally immediately after a contusion injury produced using the NYU impactor and a 25 mm weight-drop. Rats treated with VEGF showed significantly improved behavior up to 6 weeks after injury compared with control animals, while angiostatin treatment lead to no statistically significant changes in behavior outcome. Furthermore, VEGF-treated animals had an increased amount of spared tissue in the lesion center and a higher blood vessel density in parts of the wound area compared with controls. These effects were unlikely to be due to increased cell proliferation as determined by bromo-deoxy-uridine-labeling. Moreover, VEGF treatment led to decreased levels of apoptosis, as revealed by TUNEL assays. In situ hybridization demonstrated presence of mRNA for VEGF receptors Flt-1, fetal liver kinase-1, neuropilin-1 and -2 in several important cellular compartments of the spinal cord. The different experiments indicate that beneficial effects seen by acute VEGF delivery was attributable to protection/repair of blood vessels, decreased apoptosis and possibly also by other additional effects on glial cells or certain neuron populations.
机译:脊髓损伤导致急性局部缺血,这可能导致继发性变性。缺氧通过一系列事件刺激血管生成,这些事件涉及血管生成刺激物质,例如血管内皮生长因子(VEGF)。为了测试血管生成对脊髓损伤中功能性结果和伤口愈合的重要性,使用NYU撞击器和25 mm重量减轻的挫伤性损伤后立即将VEGF165(促血管生成),Ringer(对照)或血管抑素(抗血管生成)局部递送。与对照动物相比,用VEGF治疗的大鼠在受伤后长达6周时表现出明显改善的行为,而血管抑素治疗则未导致行为结果的统计学显着变化。此外,与对照组相比,用VEGF治疗的动物在病变中心的备用组织数量增加,在伤口部位的部分血管密度更高。这些作用不可能归因于通过溴脱氧尿苷标记确定的细胞增殖增加。此外,如TUNEL分析所示,VEGF治疗导致凋亡水平降低。原位杂交证明在脊髓的几个重要细胞区室中存在VEGF受体Flt-1,胎儿肝激酶-1,neuropilin-1和-2的mRNA。不同的实验表明,通过急性VEGF递送所看到的有益作用可归因于血管的保护/修复,细胞凋亡减少,还可能归因于对神经胶质细胞或某些神经元群体的其他附加作用。

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