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新纹状体纹小体神经元中脑啡肽生成不足:利用前脑啡肽-绿色荧光蛋白转基因小鼠进行的分析

Paucity of enkephalin production in neostriatal striosomal neurons: analysis with preproenkephalin-green fluorescent protein transgenic mice.

作者信息

Koshimizu Yoshinori, Wu Sheng-Xi, Unzai Tomo, Hioki Hiroyuki, Sonomura Takahiro, Nakamura Kouichi C, Fujiyama Fumino, Kaneko Takeshi

机构信息

Department of Morphological Brain Science, Graduate School of Medicine, Kyoto University, Kyoto, Japan.

出版信息

Eur J Neurosci. 2008 Nov;28(10):2053-64. doi: 10.1111/j.1460-9568.2008.06502.x.

Abstract

Whether or not the striosome compartment of the neostriatum contained preproenkephalin (PPE)-expressing neurons remained unresolved. To address this question by developing a sensitive detection method, we generated transgenic mice expressing enhanced green fluorescent protein (GFP) under the specific transcriptional control of the PPE gene. Eight transgenic lines were established, and three of them showed GFP expression which was distributed in agreement with the reported localization of PPE mRNA in the central nervous system. Furthermore, in the matrix compartment of the neostriatum of the three lines, intense GFP immunoreactivity was densely distributed in the neuronal cell bodies and neuropil, and matrix neurons displayed > 94% co-localization for GFP and PPE immunoreactivities. In sharp contrast, GFP immunoreactivity was very weak in the striosome compartment, which was characterized by intense immunoreactivity for mu-opioid receptors (MOR). Although neostriatal neurons were divided into GFP-immunopositive and -negative groups in both the striosome and matrix compartments, GFP immunoreactivity of cell bodies was much weaker (~1/5) in GFP-positive striosomal neurons than in GFP-positive matrix neurons. A similar reciprocal organization of PPE and MOR expression was also suggested in the ventral striatum, because GFP immunoreactivity was weaker in intensely MOR-immunopositive regions than in the surrounding MOR-negative regions. As PPE-derived peptides are endogenous ligands for MOR in the neostriatum and few axon collaterals of matrix neurons enter the striosome compartment, the present results raised the question of the target of those peptides produced abundantly by matrix neurons.

摘要

新纹状体的纹状体小体区是否含有表达前脑啡肽原(PPE)的神经元仍未明确。为了通过开发一种灵敏的检测方法来解决这个问题,我们构建了在PPE基因的特定转录控制下表达增强型绿色荧光蛋白(GFP)的转基因小鼠。建立了8个转基因品系,其中3个显示出GFP表达,其分布与报道的PPE mRNA在中枢神经系统中的定位一致。此外,在这3个品系新纹状体的基质区,强烈的GFP免疫反应性密集分布于神经元细胞体和神经毡中,基质神经元中GFP和PPE免疫反应性的共定位率>94%。形成鲜明对比的是,在以μ-阿片受体(MOR)强烈免疫反应性为特征的纹状体小体区,GFP免疫反应性非常弱。尽管在纹状体小体和基质区新纹状体神经元都被分为GFP免疫阳性和阴性组,但GFP阳性纹状体小体神经元细胞体的GFP免疫反应性比GFP阳性基质神经元弱得多(约为1/5)。在腹侧纹状体中也提示了PPE和MOR表达的类似反向组织,因为在MOR强烈免疫阳性区域的GFP免疫反应性比周围MOR阴性区域弱。由于PPE衍生肽是新纹状体中MOR的内源性配体,且基质神经元的轴突侧支很少进入纹状体小体区,目前的结果提出了基质神经元大量产生的这些肽的靶标的问题。

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