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Biomimetic Choline-Like Graphene Oxide Composites for Neurite Sprouting and Outgrowth

机译:仿生胆碱样氧化石墨烯复合物用于神经突发芽和生长。

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Neurodegenerative diseases or acute injuries of the nervous system always lead to neuron loss and neurite damage. Thus, the development of effective methods to repair these damaged neurons is necessary. The construction of biomimetic materials with specific physicochemical properties is a promising solution to induce neurite sprouting and guide the regenerating nerve. Herein, we present a simple method for constructing biomimetic graphene oxide (GO) composites by covalently bonding an acetylcholine-lilce unit (dimethyla- minoethyl methacrylate, DMAEMA) or phosphorylcholine- like unit (2-methacryloyloxyethyl phosphorylcholine, MPC) onto GO surfaces to enhance neurite sprouting and outgrowth. The resulting GO composites were characterized by Fourier-transform infrared spectroscopy, X-ray photoelectron spectroscopy, Raman spectroscopy, UV-vis spectrometry, scanning electron microscopy, and contact angle analyses. Primary rat hippocampal neurons were used to investigate nerve cell adhesion, spreading, and proliferation on these biomimetic GO composites. GO- DMAEMA and GO-MPC composites provide the desired biomimetic properties for superior biocompatibility without affecting cell viability. At 2 to 7 days after cell seeding was performed, the number of neurites and average neurite length on GO- DMAEMA and GO-MPC composites were significantly enhanced compared with the control GO. In addition, analysis of growth-associate protein-43 (GAP-43) by Western blot showed that GAP-43 expression was greatly improved in biomimetic GO composite groups compared to GO groups, which might promote neurite sprouting and outgrowth. All the results demonstrate the potential of DMAEMA- and MPC-modified GO composites as biomimetic materials for neural interfacing and provide basic information for future biomedical applications of graphene oxide.
机译:神经退行性疾病或神经系统的急性损伤总是导致神经元丢失和神经突损伤。因此,需要开发有效的方法来修复这些受损的神经元。具有特定物理化学性质的仿生材料的构造是诱导神经突萌发并引导再生神经的有前途的解决方案。在这里,我们提出了一种简单的方法,通过在GO表面共价键合乙酰胆碱键单元(甲基丙烯酸二甲氨基甲基乙基酯,DMAEMA)或磷胆碱样单元(2-甲基丙烯酰氧基乙基磷胆碱,MPC)来构建仿生氧化石墨烯(GO)复合物神经突发芽和长出。通过傅立叶变换红外光谱,X射线光电子能谱,拉曼光谱,紫外可见光谱,扫描电子显微镜和接触角分析来表征所得的GO复合材料。原代大鼠海马神经元用于研究这些仿生GO复合材料上神经细胞的黏附,扩散和增殖。 GO-DMAEMA和GO-MPC复合材料可提供所需的仿生特性,以实现出色的生物相容性而不会影响细胞活力。进行细胞接种后第2至7天,与对照GO相比,GO-DMAEMA和GO-MPC复合材料上的神经突数量和平均神经突长度显着增加。此外,通过蛋白质印迹分析生长相关蛋白43(GAP-43)表明,仿生GO复合组与GO组相比,GAP-43表达大大提高,这可能促进了神经突的萌发和长出。所有结果证明了DMAEMA和MPC改性的GO复合材料作为仿生材料用于神经接口的潜力,并为氧化石墨烯的未来生物医学应用提供了基本信息。

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