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首页> 外文期刊>Oncogene >p27 deficiency desensitizes Rb|[minus]||[sol]||[minus]| cells to signals that trigger apoptosis during pituitary tumor development
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p27 deficiency desensitizes Rb|[minus]||[sol]||[minus]| cells to signals that trigger apoptosis during pituitary tumor development

机译:p27缺乏使Rb | [减] || [sol] || [减] |脱敏细胞产生在垂体肿瘤发展过程中触发凋亡的信号

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摘要

Low p27 expression in many human cancers is a prognostic indicator for poor outcome. While analysing the mechanism by which p27 deficiency contributed to tumor development in the Rb+/- mouse model, we identified a role for p27 as a proapoptotic tumor suppressor. We examined the cell cycle and apoptotic response of these pituitary tumor cells to the dopamine analog bromocriptine as well as the expression of Arf and other cell cycle and apoptotic regulators in these tumors. We also examined the expression of Arf and its function in mouse embryo fibroblasts either singly or doubly deficient for Rb and p27. From these studies, we concluded that the absence of p27 disabled the trigger for an Arf-dependent apoptotic response in Rb-/- tumor cells. This suggests a novel mechanism by which the loss of p27 may impact on tumor development.
机译:许多人类癌症中p27表达低是预后不良的指标。在分析Rb +/-小鼠模型中p27缺乏导致肿瘤发展的机制时,我们确定了p27作为促凋亡性肿瘤抑制因子的作用。我们检查了这些垂体肿瘤细胞对多巴胺类似物溴隐亭的细胞周期和凋亡反应,以及这些肿瘤中Arf的表达以及其他细胞周期和凋亡调节因子。我们还检查了Arf在小鼠胚胎成纤维细胞中的表达及其功能,Rb和p27单独或双重缺陷。从这些研究中,我们得出结论,p27的缺失禁用了Rb-/-肿瘤细胞中Arf依赖性凋亡反应的触发。这表明p27的丢失可能会影响肿瘤发展的新机制。

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