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鼠源性神经移植物比人源性神经移植物更能支持大鼠的轴突再生。

Rat-derived processed nerve allografts support more axon regeneration in rat than human-derived processed nerve xenografts.

机构信息

Division of Plastic and Reconstructive Surgery, The Hospital for Sick Children, 555 University Ave, Toronto, ON, Canada M5G 1X8; Program in Physiology and Experimental Medicine, The Hospital for Sick Children Research Institute, Elizabeth McMaster Building, Toronto, ON, Canada M5G 1X8.

出版信息

J Biomed Mater Res A. 2014 Apr;102(4):1085-91. doi: 10.1002/jbm.a.34773. Epub 2013 Jun 12.

Abstract

Processed nerve allografts are increasingly used as "off the shelf" nerve replacements for surgically bridging nerve gaps. Benchmarking the regenerative capacity of a commercially available human-derived nerve or xenograft in a rat nerve injury model would provide a convenient platform for future studies seeking to modify the processed nerve graft. Human and rat processed nerve grafts were used to bridge a 14 mm defect in a Sprague-Dawley rat sciatic nerve. Reversed autografts served as a positive control group. Twelve weeks following surgery, the distal nerve stumps were retrograde labeled and harvested for histology and histomorphometry. The cross-sectional areas of the human- and rat-derived processed nerve grafts were similar. Neuron counts and myelinated axon counts following use of the human-derived processed xenografts were decreased compared with those obtained from both the rat-derived processed nerve allografts and the autografts; the rat-derived processed nerve allografts were statistically equivalent to autografts. Measures of nerve fiber diameter and myelination revealed inferior axon regeneration maturity in both processed nerve grafts compared with autografts. Processed xenografts showed significantly reduced regeneration compared with autografts or processed allografts indicating that cross-species immunological reactions are important considerations in this rat model.

摘要

处理过的同种异体神经移植物越来越多地被用作“现成的”神经替代品,用于手术桥接神经间隙。在大鼠神经损伤模型中,对市售的人源衍生神经移植物或异种移植物的再生能力进行基准测试,将为未来试图修饰处理过的神经移植物的研究提供一个便利的平台。用人和大鼠处理过的神经移植物来桥接 Sprague-Dawley 大鼠坐骨神经 14mm 的缺损。反向自体移植物作为阳性对照组。手术后 12 周,逆行标记远端神经残端并收获进行组织学和组织形态计量学分析。人源性和大鼠源性处理过的神经移植物的横截面积相似。与大鼠源性处理过的同种异体神经移植物和自体移植物相比,使用人源性处理过的异种移植物后神经元计数和有髓轴突计数减少;大鼠源性处理过的同种异体神经移植物与自体移植物在统计学上等效。神经纤维直径和髓鞘化的测量结果表明,与自体移植物相比,两种处理过的神经移植物中的轴突再生成熟度都较差。异种移植物的再生明显低于自体移植物或同种异体神经移植物,表明异种免疫反应是该大鼠模型中的重要考虑因素。

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