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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >In vivo proliferation, migration and phenotypic changes of Schwann cells in the presence of myelinated fibers.
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In vivo proliferation, migration and phenotypic changes of Schwann cells in the presence of myelinated fibers.

机译:在有髓纤维的存在下,雪旺细胞的体内增殖,迁移和表型改变。

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Following injury to a peripheral nerve, changes in the behavior of Schwann cells help to define the subsequent microenvironment for regeneration. Such changes, however, have almost exclusively been considered in the context of Wallerian degeneration distal to an injury, where loss of axonal contact or input is thought to be critical to the changes that occur. This supposition, however, may be incorrect in the proximal stumps where axons are still in contact with their cell bodies. In this work, we studied aspects of in vivo Schwann cell behavior after injury within the microenvironment of proximal stumps of transected rat sciatic nerves, where axons are preserved. In particular we studied this microenvironment proximal to the outgrowth zone, in an area containing intact myelinated fibers and a perineurial layer, by using double immunolabelling of Schwann cell markers and 5-bromo-2'-deoxyuridine (BrdU) labeling of proliferating cells.In normal sciatic nerve, Schwann cells were differentiated, in an orderly fashion, into those associated with unmyelinated fibers that labeled with glial fibrillary acidic protein (GFAP) and those associated with myelinated fibers that could be identified by individual axons and myelin sheaths. After sciatic nerve transection, there was rapid and early expansion in the population of GFAP-labeled cells in proximal stumps that was generated in part, by de novo expression of GFAP in Schwann cells of myelinated fibers. Schwann cells from this population also underwent proliferation, indicated by progressive rises in BrdU and GFAP double labeling. Finally, this Schwann cell pool also developed the property of migration, traveling to the distal outgrowth zone, but also with lateral penetration into the perineurium and epineurium, while in intimate contact with new axons.The findings suggest that other signals, in the injured proximal nerve stumps, beyond actual loss of axons, induce 'mature' Schwann cells of myelinated axons to dedifferentiate into those that up-regulated their GFAP expression, proliferate and migrate with axons.
机译:周围神经受伤后,雪旺氏细胞行为的变化有助于确定随后的再生微环境。然而,这种变化几乎完全是在损伤远端的Wallerian变性的情况下考虑的,在这种情况下,轴突接触或输入的损失对于发生的变化至关重要。但是,这种假设在轴突仍与细胞体接触的近端残端中可能是不正确的。在这项工作中,我们研究了横断大鼠坐骨神经近端残端的微环境中轴突得以保存的体内雪旺氏细胞行为的各个方面。特别是,我们通过使用Schwann细胞标记物的双重免疫标记和增殖细胞的5-bromo-2'-脱氧尿苷(BrdU)标记,在包含完整的髓鞘纤维和神经周层的区域中研究了靠近生长区的微环境。在正常的坐骨神经中,Schwann细胞以有序的方式分化为与标有神经胶质原纤维酸性蛋白(GFAP)的未髓鞘纤维相关的细胞和与可以通过单个轴突和髓鞘形成的髓鞘纤维相关的细胞。坐骨神经横断后,近端残端中GFAP标记的细胞群迅速而早期地扩张,这部分是由于在有髓纤维的雪旺细胞中从头表达GFAP而产生的。 BrdU和GFAP双重标记的进行性升高表明,该种群的雪旺细胞也经历了增殖。最后,这个Schwann细胞池还具有迁移特性,可以到达远端的生长区,而且还可以横向渗透到会阴神经和神经外膜中,同时与新的轴突紧密接触。除了轴突的实际损失之外,神经残端还诱导髓鞘轴突的“成熟”雪旺细胞分化为上调GFAP表达的细胞,并随轴突增殖和迁移。

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