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Effects of a combinatorial treatment with gene and cell therapy on retinal ganglion cell survival and axonal outgrowth after optic nerve injury

机译:组合治疗与细胞治疗对视网膜神经节细胞存活和视神经损伤后轴突产量的影响

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摘要

After an injury, axons in the central nervous system do not regenerate over large distances and permanently lose their connections to the brain. Two promising approaches to correct this condition are cell and gene therapies. In the present work, we evaluated the neuroprotective and neuroregenerative potential of pigment epithelium-derived factor (PEDF) gene therapy alone and combined with human mesenchymal stem cell (hMSC) therapy after optic nerve injury by analysis of retinal ganglion cell survival and axonal outgrowth. Overexpression of PEDF by intravitreal delivery of AAV2 vector significantly increased Tuj1-positive cells survival and modulated FGF-2, IL-1ss, Iba-1, and GFAP immunostaining in the ganglion cell layer (GCL) at 4 weeks after optic nerve crush, although it could not promote axonal outgrowth. The combination of AAV2.PEDF and hMSC therapy showed a higher number of Tuj1-positive cells and a pronounced axonal outgrowth than unimodal therapy after optic nerve crush. In summary, our results highlight a synergistic effect of combined gene and cell therapy relevant for future therapeutic interventions regarding optic nerve injury.
机译:受伤后,中枢神经系统中的轴突不会在大距离上再生,永久地失去与大脑的连接。纠正这种情况的两个有希望的方法是细胞和基因疗法。在本作本作中,我们通过分析视网膜神经节细胞存活和轴突过度,评估了单独单独的颜料上皮衍生因子(PEDF)基因治疗的神经保护和神经觅食潜力(PECF)基因治疗的神经保护和神经觅食潜力,并与视网膜神经损伤分析和轴突过多进行了视神经损伤后的人间充质干细胞(HMSC)治疗。通过玻璃体内递送Aav2载体的玻璃体内递送的过表达显着增加Tuj1阳性细胞存活和调节的FGF-2,IL-1SS,IBA-1和在视神经挤压后4周的神经节细胞层(GCl)的GFAP免疫染色,尽管它无法促进轴突过度。 AAV2.PEDF和HMSC治疗的组合显示出较多的TUJ1阳性细胞和视神经挤压后的单峰治疗的明显轴突过度。总之,我们的结果突出了对视神经损伤未来治疗干预措施相关基因和细胞疗法的协同效应。

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