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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >ErbB2 signaling in Schwann cells is mostly dispensable for maintenance of myelinated peripheral nerves and proliferation of adult Schwann cells after injury.
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ErbB2 signaling in Schwann cells is mostly dispensable for maintenance of myelinated peripheral nerves and proliferation of adult Schwann cells after injury.

机译:Schwann细胞中的ERBB2信号传导主要可用于维持损伤后的成人施旺细胞的粒细胞骨髓神经和增殖。

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摘要

Neuregulin/erbB signaling is critically required for survival and proliferation of Schwann cells as well as for establishing correct myelin thickness of peripheral nerves during development. In this study, we investigated whether erbB2 signaling in Schwann cells is also essential for the maintenance of myelinated peripheral nerves and for Schwann cell proliferation and survival after nerve injury. To this end, we used inducible Cre-loxP technology using a PLP-CreERT2 allele to ablate erbB2 in adult Schwann cells. ErbB2 expression was markedly reduced after induction of erbB2 gene disruption with no apparent effect on the maintenance of already established myelinated peripheral nerves. In contrast to development, Schwann cell proliferation and survival were not impaired in mutant animals after nerve injury, despite reduced levels of MAPK-P (phosphorylated mitogen-activated protein kinase) and cyclin D1. ErbB1 and erbB4 do not compensate for the loss of erbB2. We conclude that adult Schwann cells do not require major neuregulin signaling through erbB2 for proliferation and survival after nerve injury, in contrast to development and in cell culture.
机译:Neuregulin / ERBB信号传导至关重要,用于Schwann细胞的存活和增殖,以及在发育过程中建立正确的外周神经髓鞘厚度。在这项研究中,我们研究了Schwann细胞中的ErBB2信号是否对维持肌肉外周神经和神经损伤后的施旺细胞增殖和生存至关重要。为此,我们使用诱导的CRE-LOXP技术,使用PLP-Creert2等位基因在成人施曼细胞中烧蚀ErbB2。在诱导erbB2基因破坏后,ERBB2表达明显减少,对已经建立了粒细胞髓神经的维持无明显影响。与显影相比,由于Mapk-P(磷酸化丝裂剂活化的蛋白激酶)和细胞周期蛋白D1水平降低,氏族细胞增殖和存活率在神经损伤后不会在突变动物中损害。 erbb1和erbb4不要弥补erbb2的损失。我们得出结论,成年施旺细胞不需要通过ERBB2来通过ERBB2发出主要的Neuregulin信号,以便在神经损伤后的增殖和生存,与发育和细胞培养形成鲜明对比。

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