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Dedifferentiated Schwann cells secrete progranulin that enhances the survival and axon growth of motor neurons

机译:Deffifferentiated Schwann细胞分泌植物素,增强了运动神经元的存活率和轴突生长

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摘要

Schwann cells (SCs), the primary glia in the peripheral nervous system (PNS), display remarkable plasticity in that fully mature SCs undergo dedifferentiation and convert to repair SCs upon nerve injury. Dedifferentiated SCs provide essential support for PNS regeneration by producing signals that enhance the survival and axon regrowth of damaged neurons, but the identities of neurotrophic factors remain incompletely understood. Here we show that SCs express and secrete progranulin (PGRN), depending on the differentiation status of SCs. PGRN expression and secretion markedly increased as primary SCs underwent dedifferentiation, while PGRN secretion was prevented by administration of cAMP, which induced SC differentiation. We also found that sciatic nerve injury, a physiological trigger of SC dedifferentiation, induced PGRN expression in SCs in vivo. These results suggest that dedifferentiated SCs express and secrete PGRN that functions as a paracrine factor to support the survival and axon growth of neighboring neurons after injury.
机译:Schwann细胞(SCS),周围神经系统(PNS)中的原发性胶质胶质胶质胶质,在完全成熟的SCS中显示出显着的可塑性,经历过二草化并转化在神经损伤时进行修复SCS。 Deffifefeediated SCS通过产生增强损坏神经元的存活和轴突再生的信号来提供对PNS再生的基本支持,但神经营养因子的身份仍然不完全理解。在这里,我们表明SCS表达和分泌Progranulin(PGRN),具体取决于SCS的差异化状态。 PGRN表达和分泌显着增加,因为初级SCs接受了去消除剂,而通过营养诱导SC分化来预防PGRN分泌。我们还发现坐骨神经损伤,SC去探剂的生理触发,在体内SCS中诱导PGRN表达。这些结果表明,消化不良的SCS表达和分泌PGRN,其用作帕拉卡碱因子,以支持损伤后邻近神经元的存活和轴突生长。

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