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制备 ECM 蛋白涂覆的中空胶原通道以研究周围神经再生。

Fabrication of ECM protein coated hollow collagen channels to study peripheral nerve regeneration.

机构信息

Department of Biomedical Engineering, New Jersey Institute of Technology, Newark, NJ, 07102, USA.

出版信息

Sci Rep. 2024 Jul 12;14(1):16096. doi: 10.1038/s41598-024-67046-1.

Abstract

Peripheral nerve injury is a prevalent clinical problem that often leads to lifelong disability and reduced quality of life. Although peripheral nerves can regenerate, recovery after severe injury is slow and incomplete. The current gold standard treatment, autologous nerve transplantation, has limitations including donor site morbidity and poor functional outcomes, highlighting the need for improved repair strategies. We developed a reproducible in vitro hollow channel collagen gel construct to investigate peripheral nerve regeneration (PNR) by exploring the influence of key extracellular matrix (ECM) proteins on axonal growth and regeneration. Channels were coated with ECM proteins: collagen IV, laminin, or fibronectin and seeded with dorsal root ganglia (DRG) collected from E16 rat embryos to compare the ability of the ECM proteins to enhance axonal growth. Robust axonal extension and Schwann cell (SC) infiltration were observed in fibronectin-coated channels, suggesting its superiority over other ECM proteins. Differential effects of ECM proteins on axons and SCs indicated direct growth stimulation beyond SC-mediated guidance. In vitro laceration injury modeling further confirmed fibronectin's superior pro-regenerative effects, showcasing its potential in enhancing axonal regrowth post-injury. Advancing in vitro modeling that closely replicates native microenvironments will accelerate progress in overcoming the limitations of current nerve repair approaches.

摘要

周围神经损伤是一种常见的临床问题,常导致终身残疾和生活质量下降。尽管周围神经可以再生,但严重损伤后的恢复缓慢且不完全。目前的金标准治疗方法,自体神经移植,存在供体部位发病率高和功能预后差等局限性,这凸显了需要改进修复策略。我们开发了一种可重复的体外空心通道胶原凝胶构建体,通过探索关键细胞外基质 (ECM) 蛋白对轴突生长和再生的影响,来研究周围神经再生 (PNR)。通道涂有 ECM 蛋白:IV 型胶原、层粘连蛋白或纤连蛋白,并种植来自 E16 大鼠胚胎的背根神经节 (DRG),以比较 ECM 蛋白增强轴突生长的能力。在纤连蛋白涂层的通道中观察到了强大的轴突延伸和雪旺细胞 (SC) 浸润,表明其优于其他 ECM 蛋白。ECM 蛋白对轴突和 SC 的不同影响表明,除了 SC 介导的导向之外,还存在直接的生长刺激。体外撕裂损伤模型进一步证实了纤连蛋白优越的促再生作用,展示了其在促进损伤后轴突再生方面的潜力。推进更接近天然微环境的体外建模将加速克服当前神经修复方法局限性的进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/28a4/11245515/74aecb886195/41598_2024_67046_Fig1_HTML.jpg

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