首页> 外文期刊>ACS applied materials & interfaces >Functionalized Collagen Scaffold Neutralizing the Myelin-Inhibitory Molecules Promoted Neurites Outgrowth in Vitro and Facilitated Spinal Cord Regeneration in Vivo
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Functionalized Collagen Scaffold Neutralizing the Myelin-Inhibitory Molecules Promoted Neurites Outgrowth in Vitro and Facilitated Spinal Cord Regeneration in Vivo

机译:中和髓磷脂抑制分子的功能化胶原蛋白支架促进了神经突的体外生长并促进了脊髓的体内再生

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Research has demonstrated that many myelin-associated inhibitory molecules jointly contribute to the failure of adult spinal cord regeneration. Therapies comprehensively targeting the multiple inhibitory nature of the injured spinal cord are being concerned. Here, two collagen-binding proteins, CBD-EphA4LBD and CBD-PlexinB1LBD, were constructed, respectively, to neutralize the axon guidance molecules ephrinB3 and sema4D that inhibit the regeneration of nerve fibers. The two neutralizing proteins have proven their ability to specifically bind collagen and to continuously release from collagen scaffolds. They could also promote neurites outgrowth of cerebellar granular neurons and dorsal root ganglion neurons in vitro. Subsequently, the functionalized collagen scaffolds by physically absorbing NEP1-40 and immobilizing CBD-EphA4LBD and CBD-PlexinB1LBD were transplanted into a rat T10 complete spinal cord transection model. Our results showed that rats that received the treatment of transplanting the functionalized collagen scaffold exhibited great advantage on axonal regeneration and locomotion recovery after spinal cord injury.
机译:研究表明,许多与髓磷脂相关的抑制分子共同导致成人脊髓再生失败。人们正在关注全面针对受损脊髓的多种抑制性质的疗法。在此,分别构建了两种胶原蛋白结合蛋白CBD-EphA4LBD和CBD-PlexinB1LBD,以中和抑制神经纤维再生的轴突引导分子ephrinB3和sema4D。两种中和蛋白已证明具有特异性结合胶原蛋白并从胶原蛋白支架中连续释放的能力。它们还可以在体外促进小脑颗粒神经元和背根神经节神经元的神经突生长。随后,将通过物理吸收NEP1-40并固定CBD-EphA4LBD和CBD-PlexinB1LBD的功能化胶原蛋白支架移植到大鼠T10完整脊髓横断模型中。我们的研究结果表明,接受功能化胶原蛋白支架移植治疗的大鼠在脊髓损伤后轴突再生和运动恢复方面显示出巨大优势。

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