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正常和β2 敲除小鼠中单条视网膜传出轴突树突的发育。

Development of single retinofugal axon arbors in normal and β2 knock-out mice.

机构信息

Program in Developmental Biology, Baylor College of Medicine, Houston, Texas 77030, USA.

出版信息

J Neurosci. 2011 Mar 2;31(9):3384-99. doi: 10.1523/JNEUROSCI.4899-10.2011.

Abstract

The maturation of retinal ganglion cell (RGC) axon projections in the dorsal lateral geniculate nucleus (dLGN) and the superior colliculus (SC) relies on both molecular and activity-dependent mechanisms. Despite the increasing popularity of the mouse as a mammalian visual system model, little is known in this species about the normal development of individual RGC axon arbors or the role of activity in this process. We used a novel in vivo single RGC labeling technique to quantitatively characterize the elaboration and refinement of RGC axon arbors in the dLGN and SC in wild-type (WT) and β2-nicotinic acetylcholine receptors mutant (β2(-/-)) mice, which have perturbed retinal waves, during the developmental period when eye-specific lamination and retinotopic refinement occurs. Our results suggest that eye-specific segregation and retinotopic refinement in WT mice are not the result of refinement of richly exuberant arbors but rather the elaboration of arbors prepositioned in the proper location combined with the elimination of inappropriately targeted sparse branches. We found that retinocollicular arbors mature ∼1 week earlier than retinogeniculate arbors, although RGC axons reach the dLGN and SC at roughly the same age. We also observed striking differences between contralateral and ipsilateral RGC axon arbors in the SC but not in the LGN. These data suggest a strong influence of target specific cues during arbor maturation. In β2(-/-) mice, we found that retinofugal single axon arbors are well ramified but enlarged, particularly in the SC, indicating that activity-dependent visual map development occurs through the refinement of individual RGC arbors.

摘要

视网膜神经节细胞 (RGC) 轴突在背外侧膝状体 (dLGN) 和上丘 (SC) 中的投射的成熟依赖于分子和活动依赖性机制。尽管小鼠作为哺乳动物视觉系统模型越来越受欢迎,但在该物种中,关于单个 RGC 轴突树突的正常发育或活动在该过程中的作用知之甚少。我们使用一种新的体内单个 RGC 标记技术,在 WT 和β2-烟碱型乙酰胆碱受体突变体 (β2(-/-)) 小鼠中定量描述了 RGC 轴突树突在 dLGN 和 SC 中的发育和细化,这些小鼠的视网膜波受到干扰,在此期间发生了眼特异性分层和视敏度细化。我们的结果表明,WT 小鼠的眼特异性分离和视敏度细化不是由于丰富的树突过度细化的结果,而是由于适当位置的预先定位的树突的细化,同时消除了不合适的靶向稀疏分支。我们发现,尽管 RGC 轴突在大致相同的年龄到达 dLGN 和 SC,但视交叉节段性树突比视放射状树突成熟早约 1 周。我们还观察到在 SC 中,但不在 LGN 中,对侧和同侧 RGC 轴突树突之间存在显著差异。这些数据表明,在树突成熟过程中,目标特异性线索有很强的影响。在β2(-/-) 小鼠中,我们发现视放射状单轴突树突分支良好,但增大,特别是在 SC 中,这表明活动依赖性视觉图发育是通过单个 RGC 树突的细化来实现的。

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