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首页> 外文期刊>Acta biomaterialia >Local delivery of FK506 to injured peripheral nerve enhances axon regeneration after surgical nerve repair in rats
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Local delivery of FK506 to injured peripheral nerve enhances axon regeneration after surgical nerve repair in rats

机译:FK506的局部递送到受伤的周围神经增强了大鼠手术神经修复后的轴突再生

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摘要

Administration of FK506, an FDA approved immunosuppressant, has been shown to enhance nerve regeneration following peripheral nerve injuries. However, the severe side effects of the systemically delivered FK506 has prevented clinicians from the routine use of the drug. In this study, we analyzed the effectiveness of our fibrin gel-based FK506 delivery system to promote axon regeneration in a rat peripheral nerve transection and immediate surgical repair model. In addition, biodistribution of FK506 from the local delivery system to the surrounding tissues was analyzed in vivo. Rats in the negative control groups either did not receive any delivery system treatment or received fibrin gel with empty microspheres. The experimental groups included rats treated with fibrin gel loaded with solubilized, particulate, and poly(lactic-co-glycolic) acid microspheres-encapsulated FK506. Rats in experimental groups receiving FK506 microspheres and the particulate FK506 regenerated the highest number of motor and sensory neurons. Histomorphometric analysis also demonstrated greater numbers of myelinated axons following particulate FK506 and FK506 microspheres treatment compared to the negative control groups. In biodistribution studies, FK506 was found at the nerve repair site, the sciatic nerve, and spinal cord, with little to no drug detection in other vital organs. Hence, the local application of FK506 via our delivery systems enhanced axon regeneration whilst avoiding the toxicity of systemic FK506. This local delivery strategy represents a new opportunity for clinicians to use for cases of peripheral nerve injuries.
机译:已经显示出FK506,FK506,已显示FDA批准的免疫抑制剂,以提高周围神经损伤后的神经再生。然而,系统交付的FK506的严重副作用阻止了临床医生从药物的常规使用中。在这项研究中,我们分析了基于纤维蛋白的FK506输送系统的有效性,以促进大鼠周围神经横断和立即外科修复模型中的轴突再生。此外,在体内分析了FK506从局部递送系统到周围组织的生物分布。阴性对照组中的大鼠未接受任何递送系统处理或接受具有空微球的纤维蛋白凝胶。实验组包括用溶质,颗粒和聚(乳酸 - 共乙醇酸)酸微球的纤维蛋白凝胶处理的大鼠封装的FK506。实验组中的大鼠接受FK506微球和颗粒FK506再生最多的电动机和感官神经元。组织素质分析还显示出与阴性对照组相比,颗粒FK506和FK506微球处理后的更多数量的骨髓轴突。在生物分布研究中,FK506被发现在神经修复位点,坐骨神经和脊髓,在其他重要器官中没有任何药物检测。因此,通过我们的递送系统的局部应用FK506增强了轴突再生,同时避免了系统性FK506的毒性。本地交付策略代表了临床医生用于外周神经损伤病例的新机会。

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