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一种用于确定周围神经损伤后移植细胞促轴突生长作用的新型实验模型。

A Novel Experimental Model to Determine the Axon-Promoting Effects of Grafted Cells After Peripheral Nerve Injury.

作者信息

Endo Takeshi, Kadoya Ken, Suzuki Yuki, Kawamura Daisuke, Iwasaki Norimasa

机构信息

Department of Orthopaedic Surgery, Faculty of Medicine and Graduate School of Medicine, Hokkaido University, Sapporo, Japan.

出版信息

Front Cell Neurosci. 2019 Jun 28;13:280. doi: 10.3389/fncel.2019.00280. eCollection 2019.

Abstract

Although peripheral nerves can regenerate, clinical outcomes after peripheral nerve injuries are not always satisfactory, especially in cases of severe or proximal injuries. Further, autologous nerve grafting remains the gold standard for the reconstruction of peripheral nerves, although this method is still accompanied by issues of donor-site morbidity and limited supply. Cell therapy is a potential approach to overcome these issues. However, the optimal cell type for promoting axon regeneration remains unknown. Here, we report a novel experimental model dedicated to elucidation of the axon-promoting effects of candidate cell types using simple and standardized techniques. This model uses rat sciatic nerves and consists of a 25 mm-long acellular region and a crush site at each end. The acellular region was made by repeated freeze/thaw procedures with liquid nitrogen. Importantly, the new model does not require microsurgical procedures, which are technically demanding and greatly affect axon regeneration. To test the actual utility of this model, red fluorescent protein-expressing syngeneic Schwann cells (SCs), marrow stromal cells, or fibroblasts were grafted into the acellular area, followed by perfusion of the rat 2 weeks later. All types of grafted cells survived well. Quantification of regenerating axons demonstrated that SCs, but not the other cell types, promoted axon regeneration with minimum variability. Thus, this model is useful for differentiating the effects of various grafted cell types in axon regeneration. Interestingly, regardless of the grafted cell type, host SCs migrated into the acellular area, and the extent of axon regeneration was strongly correlated with the number of SCs. Moreover, all regenerating axons were closely associated with SCs. These findings suggest a critical role for SCs in peripheral nerve axon regeneration. Collectively, this novel experimental model is useful for elucidating the axon-promoting effects of grafted cells and for analyzing the biology of peripheral nerve axon regeneration.

摘要

尽管周围神经能够再生,但周围神经损伤后的临床效果并不总是令人满意,尤其是在严重损伤或近端损伤的情况下。此外,自体神经移植仍然是周围神经重建的金标准,尽管这种方法仍然存在供体部位发病率和供应有限的问题。细胞治疗是克服这些问题的一种潜在方法。然而,促进轴突再生的最佳细胞类型仍然未知。在此,我们报告了一种新型实验模型,该模型致力于使用简单且标准化的技术阐明候选细胞类型对轴突的促进作用。该模型使用大鼠坐骨神经,由一个25毫米长的无细胞区域和两端的挤压部位组成。无细胞区域通过液氮反复冻融程序制成。重要的是,新模型不需要显微外科手术,显微外科手术技术要求高且会极大地影响轴突再生。为了测试该模型的实际效用,将表达红色荧光蛋白的同基因雪旺细胞(SCs)、骨髓基质细胞或成纤维细胞移植到无细胞区域,两周后对大鼠进行灌注。所有类型的移植细胞均存活良好。对再生轴突的定量分析表明,SCs能促进轴突再生,且变异性最小,而其他细胞类型则不能。因此,该模型有助于区分各种移植细胞类型在轴突再生中的作用。有趣的是,无论移植的细胞类型如何,宿主SCs都会迁移到无细胞区域,并且轴突再生的程度与SCs的数量密切相关。此外,所有再生轴突都与SCs紧密相关。这些发现表明SCs在周围神经轴突再生中起关键作用。总的来说,这种新型实验模型有助于阐明移植细胞对轴突的促进作用,并分析周围神经轴突再生的生物学机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7907/6611175/d225bd1b528a/fncel-13-00280-g001.jpg

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