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Delivery of chemotropic proteins and improvement of dopaminergic neuron outgrowth through a thixotropic hybrid nano-gel

机译:通过触变杂化纳米凝胶传递趋化蛋白并改善多巴胺能神经元的生长

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摘要

Chemotropic proteins guide neuronal projections to their final target during embryo development and are useful to guide axons of neurons used in transplantation therapies. Site-specific delivery of the proteins however is needed for their application in the brain to avoid degradation and pleiotropic affects. In the present study we report the use of Poly (ethylene glycol)-Silica (PEG-Si) nanocomposite gel with thixotropic properties that make it injectable and suitable for delivery of the chemotropic protein semaphorin 3A. PEG-Si gel forms a functional gradient of semaphorin that enhances axon outgrowth of dopaminergic neurons from rat embryos or differentiated from stem cells in culture. It is not cytotoxic and its properties allowed its injection into the striatum without inflammatory response in the short term. Long term implantation however led to an increase in macrophages and glial cells. The inflammatory response could have resulted from non-degraded silica particles, as observed in biodegradation assays.
机译:趋化蛋白在胚胎发育过程中将神经元的投射引导至其最终靶标,并且可用于指导移植疗法中使用的神经元轴突。然而,蛋白质在大脑中的应用需要蛋白质的位点特异性传递,以避免降解和多效性。在本研究中,我们报告了具有触变性的聚(乙二醇)-二氧化硅(PEG-Si)纳米复合凝胶的使用,该凝胶可注射并适合递送趋化蛋白信号素3A。 PEG-Si凝胶形成信号灯蛋白的功能梯度,可增强多巴胺能神经元从大鼠胚胎或从培养的干细胞分化而来的轴突生长。它无细胞毒性,其特性使其可在短期内注射至纹状体而无炎症反应。然而,长期植入导致巨噬细胞和神经胶质细胞的增加。如在生物降解试验中观察到的,炎症反应可能是由未降解的二氧化硅颗粒引起的。

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  • 来源
    《Journal of materials science》 |2011年第9期|p.2097-2109|共13页
  • 作者单位

    Instituto de Ciencias de la Salud, Universidad Veracruzana,Av. Luis Castelazo Ayala s, 91190 Xalapa, VER, Mexico;

    Institute of Bioengineering and Nanotechnology,31 Biopolis Way, The Nanos 138669, Singapore;

    Institute of Bioengineering and Nanotechnology,31 Biopolis Way, The Nanos 138669, Singapore;

    Instituto de Neurobiologfa, Universidad Nacional Autonoma de Mexico, Blvd. Juriquilla 3001, 76230 Queretaro, QRO, Mexico;

    Centro de Fisica Aplicada y Tecnologia Avanzada, Universidad Nacional Autonoma de Mexico, Blvd. Juriquilla 3001,76230 Queretaro, QRO, Mexico;

    Instituto de Neurobiologfa, Universidad Nacional Autonoma de Mexico, Blvd. Juriquilla 3001, 76230 Queretaro, QRO, Mexico;

    Instituto de Fisiologia Celular-Neurociencias, Universidad Nacional Autonoma de Mexico, 04510 Mexico, DF, Mexico;

    Centro de Fisica Aplicada y Tecnologia Avanzada, Universidad Nacional Autonoma de Mexico, Blvd. Juriquilla 3001,76230 Queretaro, QRO, Mexico;

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