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组合式组织工程学部分恢复了脊髓损伤后的功能。

Combinatorial tissue engineering partially restores function after spinal cord injury.

机构信息

Department of Neurology, Mayo Clinic, Rochester, Minnesota, USA.

Department of Orthopedic Surgery, Mayo Clinic, Rochester, Minnesota, USA.

出版信息

J Tissue Eng Regen Med. 2019 May;13(5):857-873. doi: 10.1002/term.2840. Epub 2019 Mar 20.

Abstract

Hydrogel scaffolds provide a beneficial microenvironment in transected rat spinal cord. A combinatorial biomaterials-based strategy provided a microenvironment that facilitated regeneration while reducing foreign body reaction to the three-dimensional spinal cord construct. We used poly lactic-co-glycolic acid microspheres to provide sustained release of rapamycin from Schwann cell (SC)-loaded, positively charged oligo-polyethylene glycol fumarate scaffolds. The biological activity and dose-release characteristics of rapamycin from microspheres alone and from microspheres embedded in the scaffold were determined in vitro. Three dose formulations of rapamycin were compared with controls in 53 rats. We observed a dose-dependent reduction in the fibrotic reaction to the scaffold and improved functional recovery over 6 weeks. Recovery was replicated in a second cohort of 28 animals that included retransection injury. Immunohistochemical and stereological analysis demonstrated that blood vessel number, surface area, vessel diameter, basement membrane collagen, and microvessel phenotype within the regenerated tissue was dependent on the presence of SCs and rapamycin. TRITC-dextran injection demonstrated enhanced perfusion into scaffold channels. Rapamycin also increased the number of descending regenerated axons, as assessed by Fast Blue retrograde axonal tracing. These results demonstrate that normalization of the neovasculature was associated with enhanced axonal regeneration and improved function after spinal cord transection.

摘要

水凝胶支架可为横断大鼠脊髓提供有益的微环境。一种组合生物材料策略提供了一种微环境,促进了再生,同时减少了对三维脊髓构建体的异物反应。我们使用聚乳酸-共-羟基乙酸微球来提供雷帕霉素从负载雪旺细胞(SC)的、带正电荷的低聚聚乙二醇富马酸支架中的持续释放。单独的微球和嵌入支架中的微球的雷帕霉素的生物活性和剂量释放特性在体外进行了测定。在 53 只大鼠中,将三种剂量的雷帕霉素与对照进行了比较。我们观察到,支架的纤维化反应呈剂量依赖性降低,并且在 6 周内功能恢复得到改善。在包括重新横断损伤的第二组 28 只动物中复制了恢复。免疫组织化学和立体学分析表明,血管数量、表面积、血管直径、基底膜胶原和再生组织内的微血管表型取决于雪旺细胞和雷帕霉素的存在。TRITC-葡聚糖注射证明增强了支架通道的灌注。雷帕霉素还增加了 Fast Blue 逆行轴突追踪评估的下行再生轴突的数量。这些结果表明,新生血管的正常化与脊髓横断后轴突再生和功能改善有关。

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