首页> 外文期刊>Biomaterials >Graft of the NT-3 persistent delivery gelatin sponge scaffold promotes axon regeneration, attenuates inflammation, and induces cell migration in rat and canine with spinal cord injury
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Graft of the NT-3 persistent delivery gelatin sponge scaffold promotes axon regeneration, attenuates inflammation, and induces cell migration in rat and canine with spinal cord injury

机译:NT-3持续递送明胶海绵支架的移植促进轴突再生,减轻炎症并诱导大鼠和犬脊髓损伤的细胞迁移

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摘要

Persistent neurotrophic factor delivery is crucial to create a microenvironment for cell survival and nerve regeneration in spinal cord injury (SCI). This study aimed to develop a NT-3/fibroin coated gelatin sponge scaffold (NF-GS) as a novel controlled artificial release therapy for SCI. In vitro, bone marrow -derived mesenchymal stem cells (MSCs) were planted into the NF -GS and release test showed that NF -GS was capable to generate a sustainable NT-3 release up to 28 days. MSCs in NF -GS had high cell activity with excellent cell distribution and phenotype. Then, the NF -GS was transplanted into the injury site of spinal cord of rat and canine in vivo, which exhibited strong biocompatibility during post -transplantation period. Four weeks following transplantation, the concentration of NT-3 was much higher than that in control groups. Cavity areas in the injury/graft site were significantly reduced due to tissue regeneration and axonal extensions associated with myelin sheath through the glial scar into the NF -GS. Additionally, the NF -GS decreased the inflammation by reducing the CD68 positive cells and TNF-alpha. A striking feature was the occurrence of some cells and myelin -like structure that appeared to traverse the NF -GS. The present results demonstrate that the NF -GS has the property to control the release of NT-3 from the NT-3/fibroin complex thus facilitating regeneration of injured spinal cord. (C) 2015 Elsevier Ltd. All rights reserved.
机译:持续的神经营养因子传递对于在脊髓损伤(SCI)中为细胞存活和神经再生创造微环境至关重要。这项研究旨在开发一种NT-3 /丝蛋白包被的明胶海绵支架(NF-GS),作为SCI的新型人工控制释放疗法。在体外,将骨髓来源的间充质干细胞(MSC)植入NF -GS中,释放测试表明NF -GS能够产生可持续的NT-3释放长达28天。 NF-GS中的MSC具有高细胞活性,具有优异的细胞分布和表型。然后,NF-GS在体内被移植到大鼠和犬的脊髓损伤部位,在移植后的时期表现出很强的生物相容性。移植后四周,NT-3的浓度远高于对照组。由于组织再生和与髓鞘相关的轴突延伸穿过神经胶质瘢痕进入NF -GS,损伤/移植部位的腔区域显着减少。另外,NF -GS通过减少CD68阳性细胞和TNF-α减少了炎症。一个显着的特征是一些细胞和髓磷脂样结构的出现似乎贯穿了NF -GS。目前的结果表明,NF -GS具有控制NT-3从NT-3 /纤维蛋白复合物释放的特性,从而促进受损脊髓的再生。 (C)2015 Elsevier Ltd.保留所有权利。

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