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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Early and rapid targeting of eye-specific axonal projections to the dorsal lateral geniculate nucleus in the fetal macaque.
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Early and rapid targeting of eye-specific axonal projections to the dorsal lateral geniculate nucleus in the fetal macaque.

机译:早期和快速将眼睛特异的轴突投射物对准猕猴的背外侧膝状体核。

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The emergence of eye-specific axonal projections to the dorsal lateral geniculate nucleus (dLGN) is a well established model system for exploring the mechanisms underlying afferent targeting during development. Using modern tract tracing methods, we examined the development of this feature in the macaque, an Old World Primate with a visual system similar to that of humans. Cholera toxin beta fragment conjugated to Alexa 488 was injected into the vitreous of one eye, and CTbeta conjugated to Alexa 594 into the other eye of embryos at known gestational ages. On embryonic day 69 (E69), which is approximately 100 d before birth, inputs from the two eyes were extensively intermingled in the dLGN. However, even at this early age, portions of the dLGN were preferentially innervated by the right or left eye, and segregation is complete within the dorsalmost layers 5 and 6. By E78, eye-specific segregation is clearly established throughout the parvocellular division of the dLGN, and substantial ocular segregation is present in the magnocellular division. By E84, segregation of left and right eye axons is essentially complete, and the six eye-specific domains that characterize the mature macaque dLGN are clearly discernable. These findings reveal that targeting of eye-specific axonal projections in the macaque occurs much earlier and more rapidly than previously reported. This segregation process is completed before the reported onset of ganglion cell axon loss and retino-dLGN synapse elimination, suggesting that, in the primate, eye-specific targeting occurs independent of traditional forms of synaptic plasticity.
机译:眼特异性轴突投射到背外侧膝状核(dLGN)的出现是一个完善的模型系统,用于探索发育过程中传入靶向的机制。使用现代的道追踪方法,我们检查了猕猴(一种具有类似于人类的视觉系统的旧世界灵长类动物)中此功能的发展。将与Alexa 488结合的霍乱毒素β片段注射到已知胎龄的一只胚胎的玻璃体中,将CTbeta与Alexa 594结合的另一只眼睛注入胚胎。在出生前约100 d的胚胎第69天(E69),dLGN中广泛混入了两只眼睛的输入。然而,即使在这个很小的年龄,dLGN的部分仍优先被右眼或左眼支配,并且在最背侧的第5层和第6层内完全隔离。通过E78,在整个小细胞分裂过程中,明确建立了眼特异性隔离。 dLGN和大量的眼分离存在于大细胞分裂中。通过E84,左眼轴突和右眼轴突的分离基本完成,并且可以清楚地辨别出代表成熟猕猴dLGN的六个特定于眼睛的区域。这些发现表明,针对猕猴中眼部特定轴突投射的目标发生的时间比以前报道的要早得多,而且速度也更快。该分离过程在报道的神经节细胞轴突丧失和视网膜-dLGN突触消除发作之前完成,这表明在灵长类动物中,眼睛特异性靶向的发生独立于传统形式的突触可塑性。

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