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长期暴露于神经营养因子-3的新生大鼠新皮质长期器官型外植体中,锥体树突而非非锥体树突的生长情况。

Growth of pyramidal, but not non-pyramidal, dendrites in long-term organotypic explants of neonatal rat neocortex chronically exposed to neurotrophin-3.

作者信息

Baker R E, Dijkhuizen P A, Van Pelt J, Verhaagen J

机构信息

Netherlands Institute for Brain Research, Amsterdam.

出版信息

Eur J Neurosci. 1998 Mar;10(3):1037-44. doi: 10.1046/j.1460-9568.1998.00118.x.

DOI:10.1046/j.1460-9568.1998.00118.x
PMID:9753171
Abstract

The present study was undertaken to determine the effects of neurotrophin-3 (NT3) and spontaneous bioelectric activity (SBA) on dendritic elongation and branching in long-term isolated organotypic explants of rat neocortex. Viral vector-directed expression of NT3 was used as an effective means to ensure a continuous, local production of the neurotrophic factor. Quantitative light microscopic measurement of dendritic branching patterns was carried out on Golgi-stained materials. Explants were exposed to an adenoviral vector encoding the genetic sequence for neurotrophin-3 (Ad-NT3), or to exogenous additions of the neuropeptide NT3. In order to test for activity-dependent growth effects under control and experimental conditions, explants were exposed to glutamatergic blockade using a cocktail of APV and DNQX. Both Ad-NT3 and NT3 peptide potently promoted apical and basal dendritic growth (elongation and branching) in pyramidal neurons. This growth was observed to be significant in layers II-IV and V. These growth effects were also not activity dependent, inasmuch as they were elicited from explants in which spontaneous bioelectric activity had been suppressed. Non-pyramidal neurons, throughout the neocortical slice, showed no significant dendritic responses to the prolonged presence of NT3. These findings show that pyramidal dendritic growth in long-term neocortical explants responds to at least one neurotrophic growth factor, NT3, and is independent of intrinsic bioelectric activity. The use of viral vectors in delivering a continuous high level of neurotrophic factor within developing neural tissues demonstrates its potential application to in vivo tissues during development, or in the stimulation of neuritogenesis and neuroregeneration following injuries.

摘要

本研究旨在确定神经营养因子-3(NT3)和自发生物电活动(SBA)对大鼠新皮质长期离体器官型外植体中树突伸长和分支的影响。利用病毒载体介导的NT3表达作为确保神经营养因子持续局部产生的有效手段。对高尔基染色材料进行树突分支模式的定量光学显微镜测量。将外植体暴露于编码神经营养因子-3基因序列的腺病毒载体(Ad-NT3),或外源添加神经肽NT3。为了在对照和实验条件下测试活性依赖性生长效应,使用APV和DNQX混合物对外植体进行谷氨酸能阻断。Ad-NT3和NT3肽均有力地促进了锥体神经元顶端和基底树突的生长(伸长和分支)。在II-IV层和V层中观察到这种生长具有显著性。这些生长效应也不依赖于活性,因为它们是在自发生物电活动被抑制的外植体中引发的。整个新皮质切片中的非锥体神经元对NT3的长期存在没有明显的树突反应。这些发现表明,长期新皮质外植体中的锥体树突生长对至少一种神经营养生长因子NT3有反应,并且独立于内在生物电活动。在发育中的神经组织中使用病毒载体递送持续高水平的神经营养因子,证明了其在发育过程中对体内组织的潜在应用,或在损伤后刺激神经突生成和神经再生方面的潜在应用。

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