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促性腺激素释放激素表达 GnV-3 细胞的增殖和分化的表型和分子特征。

Phenotypic and molecular characterization of proliferating and differentiated GnRH-expressing GnV-3 cells.

机构信息

Service of Endocrinology, Diabetology and Metabolism, University Hospital and Faculty of Biology and Medicine, 1011 Lausanne, Switzerland.

出版信息

Mol Cell Endocrinol. 2011 Jan 30;332(1-2):97-105. doi: 10.1016/j.mce.2010.10.001. Epub 2010 Oct 16.

DOI:10.1016/j.mce.2010.10.001
PMID:20937356
Abstract

GnRH neurons provide the primary driving force upon the neuroendocrine reproductive axis. Here we used GnV-3 cells, a model of conditionally immortalized GnRH-expressing neurons, to perform an analysis of cell cycle and compare the gene expression profile of proliferating cells with differentiated cells. In the proliferation medium, 45 ± 1.5% of GnV-3 cells are in S-phase by FACS analysis. In the differentiation medium, only 9 ± 0.9% of them are in S-phase, and they acquire the characteristic bipolar shape displayed by preoptic GnRH neurons in vivo. In addition, GnV-3 cells in the differentiated state exhibit electrophysiological properties characteristic of neurons. Transcriptomic analysis identified up-regulation of 1931 genes and down-regulation of 1270 genes in cells grown in the differentiation medium compared to cells in the proliferation medium. Subsequent gene ontology study indicated that genes over-expressed in proliferating GnV-3 cells were mainly involved in cell cycle regulations, whereas genes over-expressed in differentiated cells were mainly involved in processes of differentiation, neurogenesis and neuronal morphogenesis. Taken together, these data demonstrate the occurrence of morphological and physiological changes in GnV-3 cells between the proliferating and the differentiated state. Moreover, the genes differentially regulated between these two different states are providing novel pathways potentially important for a better understanding of the physiology of mature GnRH neurons.

摘要

GnRH 神经元为神经内分泌生殖轴提供主要驱动力。在这里,我们使用 GnV-3 细胞,一种条件永生化 GnRH 表达神经元的模型,对细胞周期进行分析,并比较增殖细胞和分化细胞的基因表达谱。在增殖培养基中,通过 FACS 分析,45±1.5%的 GnV-3 细胞处于 S 期。在分化培养基中,只有 9±0.9%的细胞处于 S 期,它们获得了体内前脑 GnRH 神经元所显示的特征性双极形状。此外,分化状态下的 GnV-3 细胞表现出神经元的特征性电生理特性。转录组分析表明,与增殖培养基中的细胞相比,分化培养基中的细胞中上调了 1931 个基因,下调了 1270 个基因。随后的基因本体研究表明,增殖的 GnV-3 细胞中过度表达的基因主要参与细胞周期调控,而分化细胞中过度表达的基因主要参与分化、神经发生和神经元形态发生过程。总之,这些数据表明 GnV-3 细胞在增殖和分化状态之间发生了形态和生理变化。此外,这两种不同状态之间差异调节的基因为更好地理解成熟 GnRH 神经元的生理学提供了新的途径。

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