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小鼠三叉神经感觉系统中神经元的体内和体外分化与成熟

Neuronal differentiation and maturation in the mouse trigeminal sensory system, in vivo and in vitro.

作者信息

Stainier D Y, Gilbert W

机构信息

Department of Cellular and Developmental Biology, Harvard University, Cambridge, Massachusetts 02138.

出版信息

J Comp Neurol. 1991 Sep 8;311(2):300-12. doi: 10.1002/cne.903110210.

Abstract

We have isolated and characterized four monoclonal antibodies (mAbs B33, E1.9, B30, and B10) that recognize mouse trigeminal sensory neurons at specific times during development. These antibodies permit the study of neuronal differentiation, axon outgrowth, and neuronal maturation in the trigeminal sensory system. With B33, we can follow migrating neural crest and placode cells into the anlagen of the trigeminal ganglion. E1.9 immunoreactivity marks neuronal differentiation and appears in the central nervous system at embryonic day 8.5 (E8.5) and in the peripheral nervous system at E9, E1.9 and B30 show the axonal outgrowth of trigeminal sensory neurons and reveal the pioneering of the peripheral tracts by an early population of ganglionic neurons. At this stage, in the central nervous system, mesencephalic trigeminal neurons are also E1.9 and B30 positive as they migrate to their final location in the rostral metencephalon. B30 and B10 allow us to follow the maturation of these neurons. Also, in about 1% of the embryos, we identified mispositioned or misrouted trigeminal neurons. Furthermore, these biochemical markers facilitate the study of neuronal development in vitro. We find that, based on morphological and biochemical criteria, the maturation of trigeminal neurons in culture is target independent.

摘要

我们已经分离并鉴定了四种单克隆抗体(mAbs B33、E1.9、B30和B10),它们在发育过程中的特定时间识别小鼠三叉神经感觉神经元。这些抗体有助于研究三叉神经感觉系统中的神经元分化、轴突生长和神经元成熟。利用B33,我们可以追踪迁移的神经嵴和基板细胞进入三叉神经节的原基。E1.9免疫反应性标记神经元分化,在胚胎第8.5天(E8.5)出现在中枢神经系统,在E9出现在周围神经系统,E1.9和B30显示三叉神经感觉神经元的轴突生长,并揭示早期神经节神经元群体对周围神经束的开拓。在这个阶段,在中枢神经系统中,中脑三叉神经神经元在迁移到菱脑前部的最终位置时,E1.9和B30也呈阳性。B30和B10使我们能够追踪这些神经元的成熟过程。此外,在大约1%的胚胎中,我们发现了位置异常或路径错误的三叉神经神经元。此外,这些生化标记物有助于体外神经元发育的研究。我们发现,根据形态学和生化标准,培养的三叉神经神经元的成熟与靶标无关。

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