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p75 神经营养因子受体在基底前脑具有非凋亡性的抗神经营养作用。

The p75 neurotrophin receptor has nonapoptotic antineurotrophic actions in the basal forebrain.

机构信息

Department of Physiology, University of Melbourne, Parkville, Victoria, Australia.

出版信息

J Neurosci Res. 2012 Jan;90(1):278-87. doi: 10.1002/jnr.22735. Epub 2011 Sep 15.

DOI:10.1002/jnr.22735
PMID:21922519
Abstract

Because of controversy about the role of the p75 neurotrophin receptor (p75(NTR) ) in the cholinergic basal forebrain (CBF), we investigated this region in p75(NTR) third exon knockout mice that were congenic with 129/Sv controls. They express a shortened intracellular form of p75(NTR) , permitting detection of p75(NTR) -expressing cells. We performed separate counts of choline acetyltransferase (ChAT)-expressing and p75(NTR) -expressing neurons. In agreement with past reports, the number of ChAT-immunoreactive neurons in knockout mice was greater than in wild-type mice, and this was evident in each of the main anatomical divisions of the CBF. In contrast, the number of p75(NTR) -immunoreactive neurons did not differ between genotypes. The biggest increase in ChAT neurons (27%) was in the horizontal limb of the diagonal band of Broca (HDB), in which region the number of p75(NTR) -positive neurons was unchanged. Double staining revealed that some neurons in wild-type mice expressed p75(NTR) but not ChAT. In the knockout mice, all p75(NTR) -expressing neurons expressed ChAT. The increase in cholinergic neurons, therefore, was at least partially attributable to a higher proportion of ChAT immunoreactivity within the population of p75(NTR) -expressing neurons. Cholinergic neurons were also larger in knockout mice than in controls. In the hippocampal CA1 region, knockout mice had a greater number of cholinergic fibers. There was a 77% increase in hippocampal ChAT activity in knockout mice and a 38% increase in heterozygotes. The data do not support an apoptotic role but indicate a broad antineurotrophic role of p75(NTR) in the cholinergic basal forebrain.

摘要

由于 p75 神经营养因子受体 (p75(NTR))) 在胆碱能基底前脑 (CBF) 中的作用存在争议,我们研究了与 129/Sv 对照基因同源的 p75(NTR)第三外显子敲除小鼠中的这一区域。它们表达一种缩短的 p75(NTR) 细胞内形式,允许检测表达 p75(NTR) 的细胞。我们分别对胆碱乙酰转移酶 (ChAT) 表达和 p75(NTR) 表达神经元进行计数。与过去的报道一致,敲除小鼠中的 ChAT 免疫反应性神经元数量多于野生型小鼠,并且在 CBF 的每个主要解剖分区中都如此。相比之下,基因型之间的 p75(NTR) 免疫反应性神经元数量没有差异。ChAT 神经元(27%)增加最多的是 Broca 水平纹状体(HDB)的水平支,在该区域,p75(NTR) 阳性神经元数量没有变化。双重染色显示,野生型小鼠中的一些神经元表达 p75(NTR)但不表达 ChAT。在敲除小鼠中,所有表达 p75(NTR)的神经元均表达 ChAT。因此,胆碱能神经元的增加至少部分归因于表达 p75(NTR)的神经元群体中 ChAT 免疫反应性的比例更高。敲除小鼠中的胆碱能神经元也比对照小鼠中的更大。在海马 CA1 区,敲除小鼠有更多的胆碱能纤维。敲除小鼠的海马 ChAT 活性增加了 77%,杂合子增加了 38%。数据不支持凋亡作用,但表明 p75(NTR) 在胆碱能基底前脑中具有广泛的抗神经营养作用。

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