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在转基因小鼠中,生长相关蛋白B - 50/GAP - 43向嗅觉神经元的定向表达导致轴突形态和球外纤维生长的变化。

Directed expression of the growth-associated protein B-50/GAP-43 to olfactory neurons in transgenic mice results in changes in axon morphology and extraglomerular fiber growth.

作者信息

Holtmaat A J, Dijkhuizen P A, Oestreicher A B, Romijn H J, Van der Lugt N M, Berns A, Margolis F L, Gispen W H, Verhaagen J

机构信息

Netherlands Institute for Brain Research, Amsterdam-ZO, The Netherlands.

出版信息

J Neurosci. 1995 Dec;15(12):7953-65. doi: 10.1523/JNEUROSCI.15-12-07953.1995.

Abstract

B-50/GAP-43, a neural growth-associated phosphoprotein, is thought to play a role in neuronal plasticity and nerve fiber formation since it is expressed at high levels in developing and regenerating neurons and in growth cones. Using a construct containing the coding sequence of B-50/GAP-43 under the control of regulatory elements of the olfactory marker protein (OMP) gene, transgenic mice were generated to study the effect of directed expression of B-50/GAP-43 in a class of neurons that does not normally express B-50/GAP-43, namely, mature OMP-positive olfactory neurons. Olfactory neurons have a limited lifespan and are replaced throughout adulthood by new neurons that migrate into the upper compartment of the epithelium following their formation from stem cells in the basal portion of this neuroepithelium. Thus, the primary olfactory pathway is exquisitely suited to examine a role of B-50/GAP-43 in neuronal migration, lifespan, and nerve fiber growth. We find that B-50/GAP-43 expression in adult olfactory neurons results in numerous primary olfactory axons with enlarged endings preferentially located at the rim of individual glomeruli. Furthermore, ectopic olfactory nerve fibers in between the juxtaglomerular neurons or in close approximation to blood vessels were frequently observed. This suggests that expression of B-50/GAP-43 in mature olfactory neurons alters their response to signals in the bulb. Other parameters examined, that is, migration and lifespan of olfactory neurons are normal in B-50/GAP-43 transgenic mice. These observations provide direct in vivo evidence for a role of B-50/GAP-43 in nerve fiber formation and in the determination of the morphology of axons.

摘要

B-50/GAP-43是一种与神经生长相关的磷蛋白,由于其在发育和再生的神经元以及生长锥中高水平表达,被认为在神经元可塑性和神经纤维形成中发挥作用。利用一个在嗅觉标记蛋白(OMP)基因调控元件控制下包含B-50/GAP-43编码序列的构建体,培育出转基因小鼠,以研究在一类通常不表达B-50/GAP-43的神经元,即成熟的OMP阳性嗅觉神经元中定向表达B-50/GAP-43的影响。嗅觉神经元寿命有限,在成年期会被新的神经元替代,这些新神经元由神经上皮基部的干细胞形成后迁移到上皮的上部区域。因此,初级嗅觉通路非常适合用于研究B-50/GAP-43在神经元迁移、寿命和神经纤维生长中的作用。我们发现,成年嗅觉神经元中B-50/GAP-43的表达导致大量初级嗅觉轴突的末梢增大,这些末梢优先位于单个肾小球边缘。此外,经常观察到在近肾小球神经元之间或紧邻血管处有异位嗅觉神经纤维。这表明成熟嗅觉神经元中B-50/GAP-43的表达改变了它们对嗅球中信号的反应。在B-50/GAP-43转基因小鼠中,所检测的其他参数,即嗅觉神经元的迁移和寿命是正常的。这些观察结果为B-50/GAP-43在神经纤维形成和轴突形态确定中的作用提供了直接的体内证据。

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