首页> 外文期刊>European Journal of Pharmacology: An International Journal >Modulators of signal transduction pathways can promote axonal regeneration in entorhino-hippocampal slice cultures.
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Modulators of signal transduction pathways can promote axonal regeneration in entorhino-hippocampal slice cultures.

机译:信号转导途径的调节剂可以促进内嗅海马切片培养中的轴突再生。

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摘要

Axonal regeneration after lesions is usually not possible in the adult central nervous system but can occur in the embryonic and young postnatal nervous system. In this study we used the model system of mouse entorhino-hippocampal slice cultures to assess the potential of pharmacological treatments with compounds targeting signal transduction pathways to promote growth of entorhinal fibers after mechanical lesions across the lesion site to their target region in the dentate gyrus. Compounds acting on the cyclic AMP-system, protein kinase C and G-proteins have been shown before to be able to promote regeneration. In this study we have confirmed the potential of drugs affecting these systems to promote axonal regeneration in the central nervous system. In addition we have found that inhibition of the phosphoinositide 3-kinase pathway and of the inositol triphosphate receptor also promoted axonal growth across the lesion site and are thus potential novel drug targets for promoting axonal regeneration after central nervous system lesions. Our findings demonstrate that slice culture models can be used to evaluate compounds for their potential to promote axonal regeneration and that the pharmacological modulation of signal transduction pathways is a promising approach for promoting axonal repair.
机译:损伤后的轴突再生通常在成人中枢神经系统中是不可能的,但是可以在胚胎和年轻的产后神经系统中发生。在这项研究中,我们使用了小鼠内嗅海马切片培养物的模型系统,评估了靶向信号转导途径的化合物通过药理学治疗的潜力,以促进机械损伤穿过病灶部位到达齿状回的目标区域后内嗅神经纤维的生长。作用于环状AMP系统,蛋白激酶C和G蛋白的化合物已被证明能够促进再生。在这项研究中,我们已经证实了影响这些系统的药物可能会促进中枢神经系统的轴突再生。另外,我们已经发现,磷酸肌醇3-激酶途径和肌醇三磷酸受体的抑制也促进了整个病变部位的轴突生长,因此是潜在的新型药物靶标,用于促进中枢神经系统损伤后轴突再生。我们的发现表明切片培养模型可用于评估化合物促进轴突再生的潜力,并且信号转导途径的药理学调节是促进轴突修复的有前途的方法。

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