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细胞骨架调节基因在P19胚胎癌细胞加速神经突生长中的协同表达。

Coordinated expression of cytoskeleton regulating genes in the accelerated neurite outgrowth of P19 embryonic carcinoma cells.

作者信息

Bogoch Yoel, Linial Michal

机构信息

Department of Biological Chemistry, Institute of Life Sciences, The Hebrew University of Jerusalem, 91904 Israel.

出版信息

Exp Cell Res. 2008 Feb 15;314(4):677-90. doi: 10.1016/j.yexcr.2007.12.003. Epub 2007 Dec 14.

Abstract

The embryonal carcinoma P19 cells provide a model to study neuronal differentiation. Cells that are exposed to retinoic acid become mature neurons within a few days with a pronounced axonal and dendritic polarity. Notably, an accelerated rate of neurite extension characterizes densely but not sparsely plated cells. DNA microarray experiments show maximal differences in gene expression of the dense compared to sparse plated cultures at 18 h after plating. The differentially expressed genes are enriched by functions of cell adhesion and cytoskeletal regulation. Doublecortin, Lis1, Reelin, Map2 and dozens of proteins that regulate cytoskeleton dynamics increase in concordance with a rapid neurite extension. A brief elevation in intracellular cAMP via PKA is sufficient to instigate the phenotype of accelerated neurite extension with no effect on P19 cell fate. Furthermore, we show that the cAMP dependent changes in the expression of cytoskeleton regulators such as doublecortin are restricted to a short time window prior to the establishment of functional neurons. We propose that the wave of gene expression of cytoskeletal regulators that is accompanied by accelerated neurite extension acts in remodeling young developing neurons in the CNS.

摘要

胚胎癌P19细胞为研究神经元分化提供了一个模型。暴露于视黄酸的细胞在几天内会变成成熟的神经元,具有明显的轴突和树突极性。值得注意的是,神经突延伸速度加快是密集接种而非稀疏接种细胞的特征。DNA微阵列实验表明,接种后18小时,密集接种培养物与稀疏接种培养物相比,基因表达存在最大差异。差异表达的基因在细胞黏附和细胞骨架调节功能方面富集。双皮质素、Lis1、Reelin、Map2以及数十种调节细胞骨架动力学的蛋白质与神经突的快速延伸同步增加。通过蛋白激酶A短暂提高细胞内cAMP水平足以引发神经突加速延伸的表型,而对P19细胞命运没有影响。此外,我们表明,细胞骨架调节因子如双皮质素表达的cAMP依赖性变化仅限于功能性神经元建立之前的短时间窗口。我们提出,伴随着神经突加速延伸的细胞骨架调节因子基因表达浪潮,在中枢神经系统中年轻发育神经元的重塑中发挥作用。

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