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首页> 外文期刊>Biomaterials >Matrix inclusion within synthetic hydrogel guidance channels improves specific supraspinal and local axonal regeneration after complete spinal cord transection
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Matrix inclusion within synthetic hydrogel guidance channels improves specific supraspinal and local axonal regeneration after complete spinal cord transection

机译:完整的脊髓横断后,合成水凝胶引导通道中的基质包裹可改善特定的脊髓上和局部轴突再生

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摘要

We have previously shown that a novel synthetic hydrogel channel composed of poly(2-hydroxyethyl methacrylate-co-methyl methacrylate) (pHEMA-MMA) is biocompatible and supports axonal regeneration after spinal cord injury. Our goal was to improve the number and type of regenerated axons within the spinal cord through the addition of different matrices and growth factors incorporated within the lumen of the channel. After complete spinal cord transection at T8, pHEMA-MMA channels, having an elastic modulus of 263 +/- 13 kPa were implanted into adult Sprague Dawley rats. The channels were then filled with one of the following matrices: collagen, fibrin, Matrigel (TM), methylcellulose, or smaller pHEMA-MMA tubes placed within a larger pHEMA-MMA channel (called tubes within channels, TWC). We also supplemented selected matrices (collagen and fibrin) with neurotrophic factors, fibroblast growth factor-1 (FGF-1) and neurotrophin-3 (NT-3). After channel implantation, fibrin glue was applied to the cord-channel interface, and a duraplasty was performed with an expanded polytetrafluoroethylene (ePTFE (R)) membrane. Controls included animals that had either complete spinal cord transection and implantation of unfilled pHEMA-MMA channels or complete spinal cord transection. Regeneration was assessed by retrograde axonal tracing with Fluoro-Gold, and immunohistochemistry with NF-200 (for total axon counts) and calcitonin gene related peptide (CGRP, for sensory axon counts) after 8 weeks survival. Fibrin, Matrigel (TM), methylcellulose, collagen with FGF-1, collagen with NT-3, fibrin with FGF-1, and fibrin with NT-3 increased the total axon density within the channel (ANOVA,p < 0.05) compared to unfilled channel controls. Only fibrin with FGF-1 decreased the sensory axon density compared to unfilled channel controls (ANOVA, p < 0.05). Fibrin promoted the greatest axonal regeneration from reticular neurons, and methylcellulose promoted the greatest regeneration from vestibular and red nucleus neurons. With Matrige (TM), there was no axonal regeneration from brainstem motor neurons. The addition of FGF-1 increased the axonal regeneration of vestibular neurons, and the addition of NT-3 decreased the total number of axons regenerating from brainstem neurons. The fibrin and TWC showed a consistent improvement in locomotor function at both 7 and 8 weeks. Thus, the present study shows that the presence and type of matrix contained within synthetic hydrogel guidance channels affects the quantity and origin of axons that regenerate after complete spinal cord transection, and can improve functional recovery. Determining the optimum matrices and growth factors for insertion into these guidance channels will improve regeneration of the injured spinal cord. (c) 2005 Elsevier Ltd. All rights reserved.
机译:我们以前已经表明,由聚(甲基丙烯酸2-羟乙酯-甲基丙烯酸甲酯-共聚)(pHEMA-MMA)组成的新型合成水凝胶通道具有生物相容性,并在脊髓损伤后支持轴突再生。我们的目标是通过在通道内腔中添加不同的基质和生长因子来改善脊髓内再生轴突的数量和类型。在T8处完成脊髓横切后,将具有263 +/- 13 kPa弹性模量的pHEMA-MMA通道植入成年Sprague Dawley大鼠。然后在通道中填充以下基质之一:胶原蛋白,纤维蛋白,Matrigel(TM),甲基纤维素或放置在较大pHEMA-MMA通道内的较小pHEMA-MMA管(称为通道内管,TWC)。我们还用神经营养因子,成纤维细胞生长因子1(FGF-1)和神经营养蛋白3(NT-3)补充了选定的基质(胶原蛋白和纤维蛋白)。通道植入后,将纤维蛋白胶涂到脐带通道界面,并用膨体聚四氟乙烯(ePTFE(R))膜进行硬膜成形术。对照包括具有完全脊髓横断和植入未填充的pHEMA-MMA通道或完全脊髓横断的动物。存活8周后,通过用Fluoro-Gold逆行轴突追踪和NF-200(针对总轴突计数)和降钙素基因相关肽(CGRP,针对感觉轴突计数)进行免疫组织化学来评估再生。与之相比,纤维蛋白,Matrigel(TM),甲基纤维素,带有FGF-1的胶原蛋白,带有NT-3的胶原蛋白,带有FGF-1的纤维蛋白和带有NT-3的纤维蛋白增加了通道内的总轴突密度(ANOVA,p <0.05)。空的频道控件。与未填充的通道对照相比,只有具有FGF-1的纤维蛋白降低了感觉轴突密度(ANOVA,p <0.05)。纤维蛋白促进了网状神经元的最大轴突再生,甲基纤维素促进了前庭和红色核神经元的最大轴突再生。使用Matrige(TM),脑干运动神经元无轴突再生。 FGF-1的添加增加了前庭神经元的轴突再生,而NT-3的添加减少了从脑干神经元再生的轴突总数。纤维蛋白和TWC在第7和第8周均显示出运动功能的持续改善。因此,本研究表明,合成水凝胶引导通道中所含基质的存在和类型会影响完成脊髓横断后再生的轴突的数量和来源,并可以改善功能恢复。确定用于插入这些引导通道的最佳基质和生长因子将改善受伤脊髓的再生。 (c)2005 Elsevier Ltd.保留所有权利。

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