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趋化因子蛋白在小鼠脑中的定位及基因表达。

Fractalkine protein localization and gene expression in mouse brain.

作者信息

Tarozzo G, Bortolazzi S, Crochemore C, Chen S-C, Lira A S, Abrams J S, Beltramo M

机构信息

Schering-Plough Research Institute, Milan, Italy.

出版信息

J Neurosci Res. 2003 Jul 1;73(1):81-8. doi: 10.1002/jnr.10645.

Abstract

Few chemokines are expressed constitutively in the brain at detectable levels; amongst them is fractalkine. We analyzed the distribution of fractalkine in the mouse brain with the aim of giving a neuroanatomical support to the study of its physiological function. To this end, we carried out an analysis of fractalkine protein localization and gene expression. An anti-fractalkine antibody was produced and used to perform an immunohistochemical study. The results indicated a high level of fractalkine protein in cortex, hippocampus, basal ganglia, and olfactory bulb. In particular, the presence of abundant immunoreactive neurons was observed in layers II, III, V, and VI of the cortex. In the hippocampus, the CA1 region was the most intensely labeled, but immunoreactive neurons were present also in CA2 and CA3, whereas in the basal ganglia, immunoreactive cells were observed in the caudate putamen. Other brain structures such as the brainstem showed a few scattered immunoreactive cells. The presence of fractalkine immunoreactive fibers was revealed only in the olfactory bulb and in the anterior olfactory nuclei. Gene expression study results, obtained by both semiquantitative PCR and in situ hybridization, matched protein localization with the highest levels of fractalkine transcript detected in the hippocampus, cortex, and striatum. The present study showed that fractalkine protein and mRNA are constitutively expressed at a high level in forebrain structure, but are almost absent in the hindbrain. Furthermore, localization at the cellular body level would suggest a paracrine or cell-to-cell interaction role for fractalkine more than a neurotransmission modulatory function.

摘要

很少有趋化因子能在大脑中以可检测到的水平组成性表达;其中之一是fractalkine。我们分析了fractalkine在小鼠大脑中的分布,旨在为其生理功能的研究提供神经解剖学支持。为此,我们对fractalkine蛋白定位和基因表达进行了分析。制备了一种抗fractalkine抗体并用于进行免疫组织化学研究。结果表明,皮质、海马、基底神经节和嗅球中fractalkine蛋白水平较高。特别是,在皮质的II、III、V和VI层中观察到大量免疫反应性神经元。在海马中,CA1区域标记最强烈,但CA2和CA3中也存在免疫反应性神经元,而在基底神经节中,在尾状壳核中观察到免疫反应性细胞。其他脑结构如脑干显示有一些散在的免疫反应性细胞。仅在嗅球和前嗅核中发现了fractalkine免疫反应性纤维。通过半定量PCR和原位杂交获得的基因表达研究结果与蛋白定位相符,在海马、皮质和纹状体中检测到最高水平的fractalkine转录本。本研究表明,fractalkine蛋白和mRNA在前脑结构中组成性高水平表达,但在后脑中几乎不存在。此外,在细胞体水平的定位表明,fractalkine更多地发挥旁分泌或细胞间相互作用的作用,而非神经传递调节功能。

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