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首页> 外文期刊>The European Journal of Neuroscience >Insulin-like growth factor-I gene therapy increases hippocampal neurogenesis, astrocyte branching and improves spatial memory in female aging rats
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Insulin-like growth factor-I gene therapy increases hippocampal neurogenesis, astrocyte branching and improves spatial memory in female aging rats

机译:胰岛素样生长因子-I基因疗法可增强雌性衰老大鼠的海马神经发生,星形胶质细胞分支并改善空间记忆

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In rats, learning and memory performance decline during aging, which makes this rodent species a suitable model to evaluate therapeutic strategies of potential value for correcting age-related cognitive deficits. Some of these strategies involve neurotrophic factors like insulin-like growth factor-I (IGF-I), a powerful neuroprotective molecule in the brain. Here, we implemented 18-day long intracerebroventricular (ICV) IGF-I gene therapy in 28months old Sprague-Dawley female rats, and assessed spatial memory performance in the Barnes maze. We also studied hippocampal morphology using an unbiased stereological approach. Adenovectors expressing the gene for rat IGF-I or the reporter DsRed were used. Cerebrospinal fluid (CSF) samples were taken and IGF-I levels determined by radioimmunoassay. At the end of the study, IGF-I levels in the CSF were significantly higher in the experimental group than in the DsRed controls. After treatment, the IGF-I group showed a significant improvement in spatial memory accuracy as compared with DsRed counterparts. In the dentate gyrus (DG) of the hippocampus, the IGF-I group showed a higher number of immature neurons than the DsRed controls. The treatment increased hippocampal astrocyte branching and reduced their number in the hippocampal stratum radiatum. We conclude that the ependymal route is an effective approach to increase CSF levels of IGF-I and that this strategy improves the accuracy of spatial memory in aging rats. The favorable effect of the treatment on DG neurogenesis and astrocyte branching in the stratum radiatum may contribute to improving memory performance in aging rats.
机译:在大鼠中,衰老过程中的学习和记忆能力下降,这使得该啮齿动物成为适合评估潜在价值的治疗策略的模型,该策略可纠正与年龄有关的认知缺陷。这些策略中的一些涉及神经营养因子,例如胰岛素样生长因子-I(IGF-I),它是大脑中一种强大的神经保护分子。在这里,我们在28个月大的Sprague-Dawley雌性大鼠中实施了18天长的脑室内(ICV)IGF-I基因治疗,并评估了Barnes迷宫中的空间记忆性能。我们还使用无偏立体学方法研究了海马形态。使用表达大鼠IGF-1基因或报道基因DsRed的腺载体。采集脑脊液(CSF)样品,并通过放射免疫测定法测定IGF-I水平。在研究结束时,实验组脑脊液中的IGF-I水平显着高于DsRed对照组。治疗后,与DsRed对应组相比,IGF-I组显示出空间记忆准确度的显着提高。在海马的齿状回(DG)中,IGF-I组的未成熟神经元数量比DsRed对照组高。该处理增加了海马星形胶质细胞的分支,并减少了海马放射状层中海马星形胶质细胞的数量。我们得出结论,室间隔途径是增加CSF IGF-I的脑脊液水平的有效方法,并且该策略可提高衰老大鼠的空间记忆准确性。该治疗对放射状的DG神经发生和星形胶质细胞分支的有利作用可能有助于改善衰老大鼠的记忆性能。

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