首页> 外文期刊>Journal of cellular biochemistry. >The potential role of ribosomal protein S5 on cell cycle arrest and initiation of murine erythroleukemia cell differentiation.
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The potential role of ribosomal protein S5 on cell cycle arrest and initiation of murine erythroleukemia cell differentiation.

机译:核糖体蛋白S5在细胞周期停滞和启动鼠红白血病细胞分化中的潜在作用。

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Evidence now exists to indicate that some ribosomal proteins besides being structural components of the ribosomal subunits are involved in the regulation of cell differentiation and apoptosis. As we have shown earlier, initiation of erythroid differentiation of murine erythroleukemia (MEL) cells is associated with transcriptional inactivation of genes encoding ribosomal RNAs and ribosomal proteins S5 (RPS5) and L35a. In this study, we extended these observations and investigated whether transfection of MEL cells with RPS5 cDNA affects the onset of initiation of erythroid maturation and their entrance in cell cycle arrest. Stably transfected MEL cloned cells (MEL-C14 and MEL-C56) were established and assessed for their capacity to produce RPS5 RNA transcript and its translated product. The impact of RPS5 cDNA transfection on the RPS5 gene expression patterns and the accumulation of RPS5 protein in inducible transfected MEL cells were correlated with their ability to: (a) initiate differentiation, (b) enter cell cycle arrest at G(1)/G(0) phase, and (c) modulate the level of cyclin-dependent kinases CDK2, CDK4, and CDK6. The data presented indicate that deregulation of RPS5 gene expression (constitutive expression) affects RPS5 protein level and delays both the onset of initiation of erythroid maturation and entrance in cell cycle arrest in inducer-treated MEL cells.
机译:现在有证据表明,某些核糖体蛋白除了是核糖体亚基的结构成分外,还参与细胞分化和凋亡的调控。正如我们先前所显示的,鼠红细胞白血病(MEL)细胞红系分化的开始与编码核糖体RNA和核糖体蛋白S5(RPS5)和L35a的基因的转录失活有关。在这项研究中,我们扩展了这些观察结果,并研究了RPS5 cDNA转染MEL细胞是否影响红系成熟的起始及其进入细胞周期阻滞的过程。建立稳定转染的MEL克隆细胞(MEL-C14和MEL-C56),并评估其产生RPS5 RNA转录本及其翻译产物的能力。 RPS5 cDNA转染对RPS5基因表达模式的影响以及RPS5蛋白在可诱导转染的MEL细胞中的积累与它们的能力相关:(a)启动分化,(b)以G(1)/ G进入细胞周期停滞(0)阶段和(c)调节细胞周期蛋白依赖性激酶CDK2,CDK4和CDK6的水平。所提供的数据表明,RPS5基因表达(组成型表达)的失调会影响RPS5蛋白的水平,并延迟红细胞成熟的开始以及诱导剂处理的MEL细胞中细胞周期停滞的进入。

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