首页> 美国卫生研究院文献>The Journal of Neuroscience >Developmental factors affecting regeneration in the central nervous system: early but not late formed mitral cells reinnervate olfactory cortex after neonatal tract section
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Developmental factors affecting regeneration in the central nervous system: early but not late formed mitral cells reinnervate olfactory cortex after neonatal tract section

机译:影响中枢神经系统再生的发育因素:早期但不是晚期形成的二尖瓣细胞可在神经束切开后重新刺激嗅觉皮层

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摘要

If the lateral olfactory tract (LOT) of the golden hamster is transected in the first week of postnatal life, axons will grow back through the cut and reinnervate the terminal regions. Functional recovery occurs only when the terminal regions are reinnervated. The experiments reported here tested the hypothesis that reinnervation is due to neogenesis: the continued growth of newly formed axons which were not severed by the lesion. In the first experiment the birth dates of the mitral and tufted cells were determined in the hamster. It was found that mitral cells are formed on gestational days 11 and 12 (E11 and E12) and tufted cells on E11 to E14. Experiment 2 involved the combination of [3H]thymidine labeling, for the time of cell formation, with the retrograde transport of horseradish peroxidase (HRP), at a time when the LOT projections are not yet complete. The axons of early formed cells were found to reach the olfactory cortex before those of later formed cells. Experiment 3 examined the possibility that the axons which grow through an early LOT transection are new axons that had not yet reached the level of the cut. Animals were given [3H]thymidine to label the times of formation of mitral and tufted cells and then were given a transection of the LOT on postnatal day 3 (P3). After a recovery period sufficient to allow axonal regrowth and reinnervation, HRP was placed in the olfactory projection region caudal to the prior LOT section. The original hypothesis was not supported. Cells that are formed early and send out their axons early are able to reinnervate the olfactory cortex, whereas late formed cells do not. The results of this experiment suggest that the factors which prevent the regrowth of axons when the LOT is cut after P7 may depend on the stage of development of the tissue into which the axons are growing, rather than in the cells of origin and their axons.
机译:如果在出生后的第一周横切金色仓鼠的嗅觉外侧横线,轴突将通过切口长回来,并重新激活末端区域。仅当重新激活末端区域时才发生功能恢复。此处报道的实验验证了神经支配是由于新生而产生的假说:新形成的轴突的持续生长并未被病变割断。在第一个实验中,在仓鼠中确定二尖瓣和簇状细胞的出生日期。发现在妊娠第11和12天(E11和E12)形成二尖瓣细胞,在E11至E14形成簇状细胞。实验2涉及在细胞形成时[3H]胸苷标记与辣根过氧化物酶(HRP)逆行转运的结合,而LOT的预测尚未完成。发现较早形成的细胞的轴突先到达嗅皮层。实验3检验了通过早期LOT横切生长的轴突是尚未达到切口水平的新轴突的可能性。给予动物[3H]胸苷标记二尖瓣和簇状细胞的形成时间,然后在出生后第3天将其横切。在足以允许轴突再生和神经支配的恢复期之后,将HRP放置在前一个LOT段尾部的嗅觉投射区域。不支持原始假设。较早形成并提前发出轴突的细胞能够使神经皮层恢复神经,而较晚形成的细胞则不能。该实验的结果表明,在P7之后切下LOT时阻止轴突再生的因素可能取决于轴突生长所在组织的发育阶段,而不是起源细胞及其轴突。

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