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血管内皮生长因子对脱细胞神经移植物中神经再生的影响。

Effects of vascular endothelial growth factor on nerve regeneration in acellular nerve grafts.

作者信息

Rovak Jason M, Mungara Anil K, Aydin Mustafa A, Cederna Paul S

机构信息

Duke University Medical School, Durham, NC, USA.

出版信息

J Reconstr Microsurg. 2004 Jan;20(1):53-8. doi: 10.1055/s-2004-818050.

Abstract

The purpose of this study was to evaluate the effects of human recombinant vascular endothelial growth factor (VEGF-165) on peripheral nerve axonal sprouting and elongation following peripheral nerve injury and repair. Two-centimeter nerve gaps were created in rat peroneal nerves and repaired with either peripheral nerve autografts, acellular peripheral nerve isografts, or VEGF-165-treated acellular peripheral nerve isografts. Four months postoperatively, the peroneal nerves were harvested and histomorphometric analysis was performed. The reinnervated extensor digitorum longus (EDL) muscles were harvested and weighed. At the proximal nerve gap coaptation site, there was a statistically significant increase in the total number of axons and percent neural tissue in the VEGF-treated acellular nerve graft group, compared with the acellular peripheral nerve isograft and autograft groups. At the distal coaptation site, however, the total number of axons and percent neural tissue was similar in the acellular and VEGF-treated groups, which was significantly less than the autograft group. VEGF-165 treatment of acellular nerve grafts resulted in greater EDL muscle masses than acellular nerve grafts alone. VEGF treatment of acellular peripheral nerve isografts enhances axonal sprouting, resulting in an increased number of axons and percent neural tissue at the proximal nerve graft coaptation site. In the absence of any cellular elements, VEGF-impregnated acellular peripheral nerve grafts do not demonstrate enhanced axonal elongation, as noted by relatively few axons at the distal nerve graft coaptation site.

摘要

本研究的目的是评估人重组血管内皮生长因子(VEGF-165)对周围神经损伤和修复后周围神经轴突发芽和伸长的影响。在大鼠腓神经中创建2厘米的神经间隙,并用周围神经自体移植、脱细胞周围神经同种异体移植或VEGF-165处理的脱细胞周围神经同种异体移植进行修复。术后4个月,收获腓神经并进行组织形态计量分析。收获并称重重新神经支配的趾长伸肌(EDL)。在近端神经间隙吻合部位,与脱细胞周围神经同种异体移植组和自体移植组相比,VEGF处理的脱细胞神经移植组的轴突总数和神经组织百分比有统计学显著增加。然而,在远端吻合部位,脱细胞组和VEGF处理组的轴突总数和神经组织百分比相似,明显低于自体移植组。与单独的脱细胞神经移植相比,VEGF-165处理脱细胞神经移植可使EDL肌肉质量更大。VEGF处理脱细胞周围神经同种异体移植可增强轴突发芽,导致近端神经移植吻合部位的轴突数量和神经组织百分比增加。在没有任何细胞成分的情况下,VEGF浸渍的脱细胞周围神经移植并未显示出增强的轴突伸长,如远端神经移植吻合部位的轴突相对较少所示。

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