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Acidic and basic fibroblast growth factors promote stable neurite outgrowth and neuronal differentiation in cultures of PC12 cells

机译:酸性和碱性成纤维细胞生长因子促进PC12细胞培养物中神经突的稳定生长和神经元分化

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摘要

Acidic (aFGF) and basic (bFGF) fibroblast growth factors are well- characterized peptide hormones that have potent angiogenic activity and that are mitogenic for a variety of cell types. The present findings demonstrate that FGFs can reproduce the entire spectrum of rat pheochromocytoma PC12 cell responses previously shown to be elicited by NGF. These include responses that are rapid (cell flattening, enhanced phosphorylation of tyrosine hydroxylase) or delayed (neurite outgrowth, induction of phosphorylated MAP 1.2, regulation of NILE and Thy-1 glycoproteins, cessation of mitosis, elevation of AChE activity), as well as responses that have been shown to be either transcription- independent (neurite regeneration, promotion of survival) or transcription-dependent (priming, regulation of NILE and Thy-1 glycoproteins, elevation of AChE activity). The only responses for which the FGFs and NGF consistently showed quantitative differences were in the rates for neurite initiation and elongation in serum- containing medium. Thus, while all 3 factors promoted the formation of stable neurites, the network of outgrowth elicited by NGF at any given time of treatment was always of greater density. Togari et al. (1985) have previously reported that bFGF can initiate transient neurite formation in PC12 cell cultures. The present observations describe a variety of additional actions of bFGF on a neuronal cell line, and demonstrate that aFGF is capable of mimicking many, if not all, of these actions. These observations thus extend the range of actions that aFGF and bFGF may potentially exert on nerve cells, either during their development, repair, or maintenance. In addition, this work suggests that the PC12 cell line may serve as a useful model system with which to study the mechanism of action of FGFs on neurons. Since all 3 factors appear capable of eliciting the same wide spectrum of responses, molecular events specifically associated with FGFs and NGF in PC12 cells may prove illuminating of the causal steps involved in neuronal differentiation.
机译:酸性(aFGF)和碱性(bFGF)成纤维细胞生长因子是特征明确的肽激素,具有强大的血管生成活性,并且对多种细胞类型均具有促有丝分裂作用。本研究结果表明,FGFs可以复制大鼠嗜铬细胞瘤PC12细胞反应的整个光谱,先前显示是由NGF引起的。这些反应包括快速的反应(细胞扁平化,酪氨酸羟化酶的磷酸化增强)或延迟的反应(神经突向外生长,磷酸化MAP 1.2的诱导,NILE和Thy-1糖蛋白的调节,有丝分裂的停止,AChE活性的升高)以及已经显示出与转录无关的反应(神经突再生,促进存活)或与转录有关的反应(引发,NILE和Thy-1糖蛋白的调节,AChE活性的升高)。 FGF和NGF始终显示出定量差异的唯一反应是在含血清的培养基中神经突起始和伸长的速率。因此,尽管所有这三个因素都促进了稳定的神经突的形成,但在任何给定的治疗时间,NGF引起的外生网络始终具有更高的密度。 Togari等。 (1985)以前报道bFGF可以启动PC12细胞培养中的瞬时神经突形成。本观察结果描述了bFGF对神经元细胞系的多种附加作用,并证明aFGF能够模仿许多(即使不是全部)这些作用。因此,这些观察结果扩展了aFGF和bFGF在其发育,修复或维持过程中可能对神经细胞施加的作用范围。此外,这项工作表明PC12细胞系可以用作研究FGF对神经元作用机制的有用模型系统。由于所有这三个因素似乎都能够引起相同的广谱反应,因此与PC12细胞中FGF和NGF特别相关的分子事件可能证明对神经元分化所涉及的因果步骤有所启发。

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