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一种碳水化合物表位在皮层发育中对传入和传出轴突的双重作用。

Dual action of a carbohydrate epitope on afferent and efferent axons in cortical development.

作者信息

Henke-Fahle S, Mann F, Götz M, Wild K, Bolz J

机构信息

Department of Ophthalmology, University of Tübingen, Germany.

出版信息

J Neurosci. 1996 Jul 1;16(13):4195-206. doi: 10.1523/JNEUROSCI.16-13-04195.1996.

Abstract

During development of the mammalian cerebral cortex, ingrowing afferents from the thalamus take a path that is different from that of axons leaving the cortical plate. Thalamic axons arrive at the cortex at the time before their target cells of layer 4 are generated in the ventricular zone, but they invade the cortex only shortly before these cells have migrated to their final position in the cortex. Growth-promoting molecules are up-regulated in the developing cortical plate during this period. To identify such molecules, we have generated monoclonal antibodies against membrane preparations from rat postnatal cortex. In Western blots, one antibody (mAb 10) recognized a carbohydrate epitope of a glycoprotein with an apparent molecular weight extending from 180 to 370 kDa. Immunohistochemical staining revealed that the staining pattern of mAb 10 at embryonic stages delineates the pathway of thalamocortical axons, with only very faint labeling of the corticofugal pathway. In vitro assays in combination with time-lapse imaging indicated that mAb 10 has opposite effects on the growth of thalamic and cortical axons. The growth speed and axonal elongation of thalamic fibers on postnatal cortical membranes preincubated with mAb 10 was reduced compared with untreated cortical membranes. In contrast, cortical axons grew faster and stopped their growth less frequently after addition of mAb 10 to a cortical membrane substrate. Taken together, these results suggest that a carbohydrate moiety of a membrane-associated glycoprotein plays a role in the segregation of afferent and efferent cortical axons in the white matter. Moreover, the epitope recognized by mAb 10 might also contribute to regulation of the timing of the thalamocortical innervation at later developmental stages.

摘要

在哺乳动物大脑皮层发育过程中,来自丘脑的向内生长的传入神经所走的路径与离开皮层板的轴突不同。丘脑轴突在其第4层靶细胞在脑室区产生之前就到达了皮层,但它们仅在这些细胞迁移到皮层中的最终位置前不久才侵入皮层。在此期间,发育中的皮层板中促进生长的分子上调。为了鉴定此类分子,我们制备了针对大鼠出生后皮层膜制剂的单克隆抗体。在蛋白质免疫印迹中,一种抗体(单克隆抗体10)识别出一种糖蛋白的碳水化合物表位,其表观分子量范围为180至370 kDa。免疫组织化学染色显示,单克隆抗体10在胚胎阶段的染色模式描绘了丘脑皮质轴突的路径,而皮质传出路径的标记非常微弱。结合延时成像的体外试验表明,单克隆抗体10对丘脑和皮质轴突的生长具有相反的作用。与未处理的皮层膜相比,用单克隆抗体10预孵育的出生后皮层膜上丘脑纤维的生长速度和轴突伸长减少。相反,在向皮层膜底物中添加单克隆抗体10后,皮质轴突生长得更快,生长停止的频率更低。综上所述,这些结果表明,膜相关糖蛋白的碳水化合物部分在白质中传入和传出皮质轴突的分离中起作用。此外,单克隆抗体10识别的表位也可能有助于在发育后期调节丘脑皮质神经支配的时间。

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