髓鞘相关糖蛋白释放下的轴突再生:先锋雪旺细胞和卡哈尔巨型俱乐部的趋化作用。

Kojun Torigoe
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引用次数: 0

摘要

髓鞘相关糖蛋白(MAG),在切断轴突后从退化前的远端神经中释放,阻断芽和裸露轴突的再生。然而,包裹的轴突继续伸长并到达释放MAG的远端神经。为了通过膜模型法确定无轴突生长锥引导器的鞘状轴突的再生机制,我们在两个膜之间插入了一个用液氮(N2DS)处理的释放MAG的远端神经段,面对四天前切断的小鼠腓总神经的近端,以使轴突鞘状。术后第三天(第3天),接受银染色的轴突束向N2DS延伸,但几乎没有分支,形成称为Cajal巨棒(CGCs)的末端肿胀,充满轴突生长锥。用250pg/ml MAG或N2DS润湿的滤纸在插入两个膜之间时显示出相同的配置。这种作用在抗MAG治疗后消失;神经束在母神经附近有许多分支,形成了一个轴突网,并在其末端向细尖端逐渐变细,就像没有N2DS的对照一样。在第3天,用抗S100检测到的施旺细胞束在其末端形成CGCs的鞘,并连接到先锋施旺细胞(pSCs)。为了分析施旺细胞的生理学,独立于轴突,将四天前切断的亲代神经粉碎。在第2天,随着pSCs的到来,施旺细胞束向N2DS延伸。在第4天,主束退化,使pSCs静止不动。因此,MAG是pSCs和CGCs的候选化学引诱剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Axonal regrowth under release of myelin-associated glycoprotein: chemotaxis by pioneer Schwann cells and Cajal's gigantic clubs.

Myelin-associated glycoprotein (MAG), released from pre-degenerated distal nerves following axotomy, blocks the regrowth of sprouts and naked axons. Ensheathed axons, however, continue to elongate and reach MAG-releasing distal nerves. To determine the regenerative mechanism of ensheathed axons without navigators of axonal growth cones by the film model method, we inserted a MAG-releasing distal nerve segment treated with liquid nitrogen (N2DS) between the two films, facing the proximal end of the common peroneal nerves in mice transected 4 days earlier for axons to become ensheathed. On the third postoperative day (Day 3), axon fascicles, subjected to silver staining, extended toward N2DS but with few branches, forming terminal swellings called Cajal's gigantic clubs (CGCs) that are filled with axonal growth cones. Filter paper wetted with either 250 pg/ml MAG or N2DS showed the same configurations when inserted between the two films. This effect was lost following anti-MAG treatment; fascicles strayed near the parent nerve with numerous branches, formed a net of axons and tapered toward thin tips at their ends, just like controls without N2DS. Schwann cell bundles on Day 3 detected with anti-S100, formed sheaths of CGCs at their ends and connected to pioneer Schwann cells (pSCs). To analyze the physiology of Schwann cells, independent of axons, the parent nerve transected 4 days prior was crushed. On Day 2, with pSCs ahead, Schwann cell bundles extended toward N2DS. On Day 4, main bundles regressed, leaving pSCs motionless. Thus, MAG is a candidate chemoattractant for both pSCs and CGCs.

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