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人类纹状体内的酪氨酸羟化酶阳性神经元表达转录因子Nurr1。

Tyrosine hydroxylase-positive neurons intrinsic to the human striatum express the transcription factor Nurr1.

作者信息

Cossette Martine, Parent André, Lévesque Daniel

机构信息

Centre de recherche Université Laval Robert-Giffard, 2601 de la Canardière, Beauport (Québec), Canada G1J 2G3.

出版信息

Eur J Neurosci. 2004 Oct;20(8):2089-95. doi: 10.1111/j.1460-9568.2004.03661.x.

Abstract

The putative dopaminergic (DA) neurons intrinsic to human striatum were studied to determine their similarity with DA neurons of the substantia nigra pars compacta (SNpc). The comparison was based on morphological features and on the presence or absence of Nurr1, an orphan receptor of the nuclear receptor family that is essential for the expression of DA phenotype by developing SNpc neurons. Immunohistochemistry for the neuronal nuclear protein (NeuN; a neuronal marker) and in situ hybridization for tyrosine hydroxylase (TH) and/or Nurr1 were applied to post-mortem tissue obtained from seven normal individuals. On one hand, the TH-positive multipolar neurons in the human striatum, which were subdivided into three groups according to their size and pattern of dendritic arborization, were found to be morphologically similar to TH-positive neurons of the SNpc. The distribution frequency of striatal TH-positive neurons, according to their diameter, closely matches the frequency observed for multipolar TH-positive cells in the SNpc. On the other hand, the proportion of neurons expressing Nurr1 and TH mRNA transcripts on single striatal section was similar to the proportion of TH-immunoreactive neurons observed on adjacent sections. More importantly, in each striatum analysed, virtually all cells that stained for TH also expressed NeuN and Nurr1. This study provides novel data that confirm the existence of DA neurons intrinsic to the human striatum. It also provides the first evidence for the existence of striking morphological and chemical similarities between the DA neurons present at striatal level and those that populate the SNpc.

摘要

对人类纹状体内假定的多巴胺能(DA)神经元进行了研究,以确定它们与黑质致密部(SNpc)的DA神经元的相似性。该比较基于形态学特征以及核受体家族孤儿受体Nurr1的有无,Nurr1对于发育中的SNpc神经元表达DA表型至关重要。对从7名正常个体获取的尸检组织应用了神经元核蛋白免疫组织化学(NeuN;一种神经元标记物)以及酪氨酸羟化酶(TH)和/或Nurr1的原位杂交。一方面,发现人类纹状体内的TH阳性多极神经元根据其大小和树突分支模式可分为三组,在形态上与SNpc的TH阳性神经元相似。纹状体内TH阳性神经元的分布频率,根据其直径,与SNpc中多极TH阳性细胞观察到的频率密切匹配。另一方面,在单个纹状体切片上表达Nurr1和TH mRNA转录本的神经元比例与在相邻切片上观察到的TH免疫反应性神经元比例相似。更重要的是,在分析的每个纹状体中,几乎所有TH染色的细胞也表达NeuN和Nurr1。这项研究提供了新的数据,证实了人类纹状体内存在DA神经元。它还首次证明了纹状体水平的DA神经元与构成SNpc的DA神经元之间存在显著的形态和化学相似性。

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