人前列腺细胞不依赖p53的致瘤进展。

P Ramsamooj, M Kuettel, A Dritschilo, M Jung
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引用次数: 2

摘要

我们之前已经描述了辐射转化的人类胎儿前列腺上皮细胞267B1的发育。利用该体外模型系统,我们通过比较非致瘤性(267B1/B)和致瘤性(267B1/D)细胞来研究前列腺癌进展的分子机制。我们在同步细胞中检测了G1期到s期的转变,以确定267B1细胞从非致瘤性到致瘤性的进展是否是G1期到s期转变中涉及p53、pRb、p21或p16的扰动的结果。非致瘤性267B1/B细胞在暴露于电离辐射(6 Gy)后表现出p53表达的时间依赖性增加和p21表达的相应增加。pRb和p16蛋白的水平几乎没有变化。相比之下,致瘤性267B1/D细胞在电离辐射的作用下表现出不依赖p53的p21蛋白诱导,p16蛋白平行增加,但pRb没有变化。这些结果表明,267B1细胞从非致瘤性到致瘤性的过程涉及p53独立的过程。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
p53-Independent tumorigenic progression of human prostate cells.

We have previously described the development of radiation transformed human fetal prostate epithelial cells, 267B1. Using this in vitro model system, we investigated the molecular mechanisms of prostate carcinogenic progression by comparing nontumorigenic (267B1/B) and tumorigenic (267B1/D) cells. We examined the G1- to S-phase transition in synchronized cells to determine if the progression of 267B1 cells from nontumorigenic to tumorigenic was the consequence of a perturbation in the G1- to S-phase transition involving p53, pRb, p21, or p16. Nontumorigenic 267B1/B cells showed a time-dependent increase in the expression of p53 and a corresponding increase in p21 following exposure to ionizing radiation (6 Gy). The levels of pRb and p16 protein were virtually unchanged. In contrast, tumorigenic 267B1/D cells exhibited a p53-independent induction of p21 protein with a parallel increase in p16 protein in response to ionizing radiation, but no change in pRb was observed. These results suggest that the progression of 267B1 cells from nontumorigenic to tumorigenic involves p53-independent processes.

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