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Rab8a/Rab11a regulate intercellular communications between neural cells via tunneling nanotubes

机译:Rab8a / Rab11a通过隧道纳米管调节神经细胞之间的细胞间通信

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Tunneling nanotubes (TNTs) are F-actin-based membrane tubes, and can form between cultured cells and within vital tissues. TNTs mediate intercellular communications that range from electrical signaling to the transfer of organelles. Following peripheral nerve injury, the orchestrated intercellular communications among neural and non-neural cells are required for effective nerve regeneration. It remains unknown whether TNTs exist between neural cells in the peripheral nerve system and how TNTs affect neural regeneration. To address these interesting questions, we investigated the transfer of neurotropic factors, membrane protein, cytoplasmic protein, mitochondria and RNA in functional TNTs formed between cultured Schwann cells (SCs). TNT-like structures were increased not only in cultured SCs after exposure to serum depletion but also in longitudinal sections of proximal sciatic nerve stump harvested after rat peripheral nerve transection. Meanwhile, downregulation of Rab8a or Rab11a in cultured SCs inhibited the formation of functional TNTs and vesicle transfer and led to decrease in cell migration, increase in SCs apoptosis. Likewise, knockdown of Rab8a or Rab11a in primary SCs also suppressed axonal outgrowth from co-cultured dorsal root ganglion (DRG) neurons. Overall, our results suggested that the gene of Rab8a or Rab11a might be involved in the formation of TNTs structures in the peripheral nerve system, while TNTs structures were likely to affect peripheral nerve regeneration through the regulation of neural cell communications.
机译:隧道纳米管(TNT)是基于F-肌动蛋白的膜管,可以在培养的细胞和重要组织内形成。 TNT介导的间细胞间通信范围从电信带到细胞器的转移。在周围神经损伤之后,需要治疗神经细胞之间的策划的细胞间通信,需要有效的神经再生。仍然未知是否存在TNT在周围神经系统中的神经细胞之间以及TNT如何影响神经再生。为了解决这些有趣的问题,我们调查了在培养的施旺细胞(SCS)之间形成的功能性TNT中的神经渗透因子,膜蛋白,细胞质蛋白,线粒体和RNA的转移。在暴露于血清耗尽后的培养SCs中,而且在大鼠周围神经横衰竭之后收获的近侧坐骨神经树桩的纵向部分,不仅在培养的SCs中增加了TNT的结构。同时,培养SCS中Rab8a或Rab11a的下调抑制了功能性TNT和囊泡转移的形成,并导致细胞迁移降低,SCS细胞凋亡增加。同样地,rab8a或rab11a在初级scs中的敲低也抑制了共培养的背根神经节(DRG)神经元的轴突产量。总体而言,我们的结果表明RAB8A或RAB11A的基因可能参与外周神经系统中TNTS结构的形成,而TNTS结构可能通过对神经细胞通信的调节影响外周神经再生。

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