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羊水来源干细胞接种的脱细胞异体神经移植物用于周围神经再生

Peripheral Nerve Regeneration with Acellular Nerve Allografts Seeded with Amniotic Fluid-Derived Stem Cells.

作者信息

Ma Xue, Elsner Eileen, Cai Jiaozhong, Smith Thomas L, Li Zhongyu

机构信息

Department of Orthopedic Surgery, Wake Forest University School of Medicine, NC, Medical Center Boulevard, Winston-Salem, North Carolina 27157, USA.

出版信息

Stem Cells Int. 2022 Aug 1;2022:5240204. doi: 10.1155/2022/5240204. eCollection 2022.

Abstract

INTRODUCTION

Tissue engineering strategies have attempted to mimic regenerating axons' environment by adding supportive types of cells other than Schwann cell to the nerve allograft. We hypothesized that allografts can be seeded with amniotic fluid-derived stem cells (AFS) to promote nerve regeneration.

METHODS

ANAs with AFS cells for long-gap nerve repairs were studied using a rat model. A sciatic nerve injury was created and repaired immediately with a rat acellular nerve allograft (ANA) construct alone, an ANA construct seeded with AFS cells, or with an autograft. Walking track analysis and electrophysiology were performed to document the return of motor control at 4 months post injury. Axon morphology on the nerve segments was assessed.

RESULTS

gait analysis showed that the ANA plus AFS cell group had significantly advanced recoveries in overlap distance, paw angle degree, paw drag, stance width, axis distance, and sciatic function index (SFI) compared with ANA alone. The ANA plus AFS cell group also demonstrated greater gastrocnemius compound muscle action potential (CMAP) ratio, sciatic axon diameter, fiber diameter, myelin thickness, ratio (average axonal diameter (AD)/fiber diameter (FD)), and neuromuscular junction (NMJ) numbers compared to ANA. . The allograft plus AFS cell group demonstrated significantly improved functional and histological outcomes compared to allograft group alone, showing no significant difference of the nerve regeneration from the autograft group. Thus, AFS cells may be a suitable cell source to replace Schwann cells to support and accelerate peripheral nerve regeneration following large-gap nerve injury.

摘要

引言

组织工程策略试图通过在神经同种异体移植物中添加除雪旺细胞之外的支持性细胞类型来模拟再生轴突的环境。我们假设同种异体移植物可以接种羊水来源的干细胞(AFS)以促进神经再生。

方法

使用大鼠模型研究接种AFS细胞用于长间隙神经修复的无细胞神经同种异体移植物(ANA)。制造坐骨神经损伤,然后分别用单独的大鼠无细胞神经同种异体移植物(ANA)构建体、接种AFS细胞的ANA构建体或自体移植物立即进行修复。在损伤后4个月进行行走轨迹分析和电生理学检查,以记录运动控制的恢复情况。评估神经节段上的轴突形态。

结果

步态分析表明,与单独使用ANA相比,ANA加AFS细胞组在重叠距离、爪角度、爪拖曳、站立宽度、轴距离和坐骨神经功能指数(SFI)方面的恢复明显提前。与ANA相比,ANA加AFS细胞组还表现出更大的腓肠肌复合肌肉动作电位(CMAP)比率、坐骨神经轴突直径、纤维直径、髓鞘厚度、比率(平均轴突直径(AD)/纤维直径(FD))和神经肌肉接头(NMJ)数量。与单独的同种异体移植物组相比,同种异体移植物加AFS细胞组的功能和组织学结果有显著改善,显示与自体移植物组的神经再生无显著差异。因此,AFS细胞可能是一种合适的细胞来源,可替代雪旺细胞以支持和加速大间隙神经损伤后周围神经的再生。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eca2/9359847/a1edba6f2cee/SCI2022-5240204.001.jpg

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