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首页> 外文期刊>CNS neuroscience & therapeutics. >RNAi‐mediated ephrin‐B2 silencing attenuates astroglial‐fibrotic scar formation and improves spinal cord axon growth
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RNAi‐mediated ephrin‐B2 silencing attenuates astroglial‐fibrotic scar formation and improves spinal cord axon growth

机译:RNAi介导的ephrin-B2沉默可减轻星形胶质纤维化疤痕的形成并改善脊髓轴突的生长

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Summary AimsAstroglial-fibrotic scar formation following central nervous system injury can help repair blood-brain barrier and seal the lesion, whereas it also represents a strong barrier for axonal regeneration. Intensive preclinical efforts have been made to eliminate/reduce the inhibitory part and, in the meantime, preserve the beneficial role of astroglial-fibrotic scar. MethodsIn this study, we established an in vitro system, in which coculture of astrocytes and meningeal fibroblasts was treated with exogenous transforming growth factor-β1 (TGF-β1) to form astroglial-fibrotic scar-like cell clusters, and thereby evaluated the efficacy of RNAi targeting ephrin-B2 in preventing scar formation from the very beginning. We further tested the effect of RNAi-based mitigation of astroglial-fibrotic scar on spinal axon outgrowth on a custom-made microfluidic platform. ResultsWe found that siRNA targeting ephrin-B2 significantly reduced both the number and the diameter of cell clusters induced by TGF-β1 and diminished the expression of aggrecan and versican in the coculture, and allowed for significantly longer extension of outgrowing spinal cord axons into astroglial-fibrotic scar as assessed on the microfluidic platform. ConclusionsThese results suggest that astroglial-fibrotic scar formation and particularly the expression of aggrecan and versican could be mitigated by ephrin-B2 specific siRNA, thus improving the microenvironment for spinal axon regeneration.
机译:总结目的中枢神经系统损伤后星形胶质纤维化疤痕的形成可以帮助修复血脑屏障并密封病变,而它也代表了轴突再生的强大屏障。为了消除/减少抑制部分并同时保持星形胶质纤维化瘢痕的有益作用,已经进行了深入的临床前努力。方法在本研究中,我们建立了一个体外系统,其中星形胶质细胞和脑膜成纤维细胞的共培养物通过外源转化生长因子-β1(TGF-β1)处理形成星形胶质纤维化瘢痕样细胞簇,从而评估了其有效性。从一开始就靶向ephrin-B2的RNAi可以防止疤痕形成。我们进一步测试了基于RNAi的星形胶质纤维化瘢痕缓解对定制微流控平台上脊髓轴突生长的影响。结果我们发现靶向ephrin-B2的siRNA显着减少了TGF-β1诱导的细胞簇的数量和直径,并减少了共培养中聚集蛋白聚糖和versican的表达,并允许更长的脊髓轴突延伸成星形胶质细胞。如在微流体平台上评估的纤维化瘢痕。结论这些结果表明,通过ephrin-B2特异性siRNA可以减轻星形胶质纤维化疤痕的形成,特别是聚集蛋白聚糖和versican的表达,从而改善脊髓轴突再生的微环境。

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