School of Chemical and Biomedical Engineering, Nanyang Technological University, Singapore, Singapore.
Tissue Eng Part A. 2012 May;18(9-10):1057-66. doi: 10.1089/ten.TEA.2011.0430. Epub 2012 Feb 8.
Nerve regeneration in an injured spinal cord is often restricted, contributing to the devastating outcome of neurologic impairment below the site of injury. Although implantation of tissue-engineered scaffolds has evolved as a potential treatment method, the outcomes remain sub-optimal. One possible reason may be the lack of topographical signals from these constructs to provide contact guidance to invading cells or regrowing axons. Nanofibers mimic the natural extracellular matrix architecturally and may therefore promote physiologically relevant cellular phenotypes. In this study, the potential application of electrospun collagen nanofibers (diameter=208.2±90.4 nm) for spinal cord injury (SCI) treatment was evaluated in vitro and in vivo. Primary rat astrocytes and dorsal root ganglias (DRGs) were seeded on collagen-coated glass cover slips (two-dimensional [2D] substrate controls), and randomly oriented or aligned collagen fibers to evaluate scaffold topographical effects on astrocyte behavior and neurite outgrowth, respectively. When cultured on collagen nanofibers, astrocyte proliferation and expression of glial fibrillary acidic protein (GFAP) were suppressed as compared to cells on 2D controls at days 3 (p<0.05) and 7 (p<0.01). Aligned fibers resulted in elongated astrocytes (elongation factor >4, p<0.01) and directed the orientation of neurite outgrowth from DRGs along fiber axes. In the contrast, neurites emanated radially on randomly oriented collagen fibers. By forming collagen scaffolds into spiral tubular structures, we demonstrated the feasibility of using electrospun nanofibers for the treatment of acute SCI using a rat hemi-section model. At days 10 and 30 postimplantation, extensive cellular penetration into the constructs was observed regardless of fiber orientation. However, scaffolds with aligned fibers appeared more structurally intact at day 30. ED1 immunofluorescent staining revealed macrophage invasion by day 10, which decreased significantly by day 30. Neural fiber sprouting as evaluated by neurofilament staining was observed as early as day 10. In addition, GFAP immunostained astrocytes were found only at the boundary of the lesion site, and no astrocyte accumulation was observed in the implantation area at any time point. These findings indicate the feasibility of fabricating 3D spiral constructs using electrospun collagen fibers and demonstrated the potential of these scaffolds for SCI repair.
脊髓损伤后的神经再生常常受到限制,导致损伤部位以下的神经功能损伤具有破坏性。尽管组织工程支架的植入已经发展成为一种潜在的治疗方法,但结果仍然不理想。一个可能的原因是这些构建体缺乏拓扑信号,无法为侵入细胞或再生轴突提供接触指导。纳米纤维在结构上模拟天然细胞外基质,因此可能促进具有生理相关性的细胞表型。在这项研究中,评估了电纺胶原纳米纤维(直径=208.2±90.4nm)在脊髓损伤(SCI)治疗中的应用,分别在体外和体内进行了评估。将原代大鼠星形胶质细胞和背根神经节(DRGs)接种在涂有胶原的玻璃盖玻片(二维[2D]基底对照)上,以评估支架拓扑结构对星形胶质细胞行为和轴突生长的影响。与 2D 对照相比,在胶原纳米纤维上培养时,星形胶质细胞的增殖和神经丝酸性蛋白(GFAP)的表达在第 3 天(p<0.05)和第 7 天(p<0.01)时受到抑制。排列的纤维导致星形胶质细胞伸长(伸长因子>4,p<0.01),并沿纤维轴引导 DRGs 轴突的生长方向。相比之下,轴突从随机排列的胶原纤维中呈放射状发散。通过将胶原支架制成螺旋管状结构,我们使用大鼠半切模型证明了使用电纺纳米纤维治疗急性 SCI 的可行性。在植入后第 10 天和第 30 天,无论纤维取向如何,都观察到大量细胞渗透到构建体中。然而,在第 30 天,具有排列纤维的支架似乎结构更完整。ED1 免疫荧光染色显示第 10 天有巨噬细胞浸润,第 30 天显著减少。神经丝染色显示神经纤维发芽早在第 10 天就观察到。此外,仅在损伤部位边界处发现 GFAP 免疫染色的星形胶质细胞,在任何时间点都未在植入区域观察到星形胶质细胞聚集。这些发现表明使用电纺胶原纤维制造 3D 螺旋结构的可行性,并证明了这些支架用于 SCI 修复的潜力。
