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首页> 外文期刊>Experimental Gerontology >Exploration of replicative senescence-associated genes in human dermal fibroblasts by cDNA microarray technology.
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Exploration of replicative senescence-associated genes in human dermal fibroblasts by cDNA microarray technology.

机译:利用cDNA芯片技术探索人皮肤成纤维细胞中的复制衰老相关基因。

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摘要

The aging process is known to be regulated by specific genes in various organisms, including yeast, the nematode C. elegans, fruitflies and mice. To explore the novel genes involved in aging process, we applied cDNA microarray technology to a replicative senescence model of human dermal fibroblasts (HDF). Eighty-four genes, including inflammatory genes, cell cycle regulatory genes, cytoskeletal genes, and metabolic genes were found to show more than two fold expressional differences in young and old fibroblasts. Furthermore, 31 genes were confirmed to be up- or down-regulated during replicative senescence by semi-quantitative RT-PCR. The overexpressions of several genes including CD36, putative lymphocyte G0/G1 switch gene (G0S2), tumor protein D52-like 1 (TPD52L1), chemokine (C-X-C motif) ligand 6, myxovirus resistant gene 1 (MX1), and the down-regulation of the immunoglobulin superfamily containing leucine-rich repeat (ISLR), neurotrimin, insulin-like growth factor 2 associated protein (IGF2A), and apoptosis-related RNA binding protein (NAPOR3) were newly identified. These results suggest that fibroblasts show the deregulation of various cellular processes, such as inflammatory response, mitosis, cell adhesion, transport, signal transduction, and metabolism during replicative senescence.
机译:已知衰老过程受各种生物体中特定基因的调控,包括酵母,线虫秀丽隐杆线虫,果蝇和小鼠。为了探索参与衰老过程的新基因,我们将cDNA微阵列技术应用于人皮肤成纤维细胞(HDF)的复制衰老模型。发现包括发炎基因,细胞周期调节基因,细胞骨架基因和代谢基因在内的八十四个基因在年轻和老成纤维细胞中显示出超过两倍的表达差异。此外,通过半定量RT-PCR证实了31个基因在复制衰老过程中被上调或下调。 CD36,推定的淋巴细胞G0 / G1转换基因(G0S2),肿瘤蛋白D52样1(TPD52L1),趋化因子(CXC基序)配体6,粘液病毒抗性基因1(MX1)和下调等几种基因的过表达新鉴定了包含富亮氨酸重复序列(ISLR),神经蛋白,胰岛素样生长因子2相关蛋白(IGF2A)和凋亡相关RNA结合蛋白(NAPOR3)的免疫球蛋白超家族。这些结果表明成纤维细胞在复制性衰老过程中显示出各种细胞过程的失调,例如炎症反应,有丝分裂,细胞粘附,转运,信号转导和代谢。

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