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低剂量电离辐射对永生化小鼠细胞中Trp53激活的剂量和剂量率效应。

Dose and dose-rate effects of low-dose ionizing radiation on activation of Trp53 in immortalized murine cells.

作者信息

Sugihara Takashi, Magae Junji, Wadhwa Renu, Kaul Sunil C, Kawakami Yasushi, Matsumoto Tsuneya, Tanaka Kimio

机构信息

Department of Radiobiology, Institute for Environmental Sciences, 1-7 Ienomae, Obuchi, Rokkasho, Kamikita, Aomori 039-3212, Japan.

出版信息

Radiat Res. 2004 Sep;162(3):296-307. doi: 10.1667/rr3223.

Abstract

A derivative of immortalized murine NIH/PG13Luc cells stably transfected with a Trp53-dependent luciferase reporter plasmid was used to study the transcriptional activity of Trp53 in response to radiation. The cell line was sensitive enough to detect the response of Trp53 to 0.2 cGy of (60)Co gamma radiation. To examine the biological effects of low-dose-rate (60)Co gamma radiation (from 0.1-10 cGy/h), we have analyzed the cell cycle, Trp53 transcriptional activity, and gene expression profiles of control and treated cells. Microarray analysis revealed up-regulation of six Trp53-mediated genes (Cdkn1a/ p21, Mdm2, Sip27, Ccng1/cyclin G1, Ei24/Pig8 and Dinb/ Polk) after exposure of cells to low-dose-rate radiation for 72 h. Using real-time PCR, a significant elevation in the expression of Ccng1/cyclin G1, Mdm2 and Cdkn1A/p21 was observed with low-dose-rate irradiation at dose rates over 5 cGy/ h. A dose-rate dependence was also observed for these three Trp53-mediated genes. The expression of Ccng1/cyclin G1 at high dose rates of gamma rays was higher than that for low dose rate. However, the expression of Mdm2 for low-dose-rate gamma rays was higher than for the high dose rate. Cells irradiated at low dose rates of 0.1 cGy/h and 1 cGy/h underwent G(1)-phase arrest. Furthermore, G(2)-phase growth arrest was observed in cells irradiated at the low dose rates of 5 cGy/h and 10 cGy/h, which correlated with Trp53-mediated Ccng1/cyclin G1 up-regulation. These results show that cellular response to radiation depended on the dose rate used; i.e., the responses seen at dose rates from 0.1-1 cGy/h were different from those observed at dose rates over 5 cGy/h.

摘要

一种稳定转染了依赖Trp53的荧光素酶报告质粒的永生化小鼠NIH/PG13Luc细胞衍生物被用于研究Trp53对辐射的转录活性。该细胞系足够敏感,能够检测到Trp53对0.2 cGy的(60)Coγ辐射的反应。为了研究低剂量率(60)Coγ辐射(0.1 - 10 cGy/h)的生物学效应,我们分析了对照细胞和处理细胞的细胞周期、Trp53转录活性及基因表达谱。微阵列分析显示,细胞在低剂量率辐射72小时后,六个Trp53介导的基因(Cdkn1a/p21、Mdm2、Sip27、Ccng1/细胞周期蛋白G1、Ei24/Pig8和Dinb/Polk)上调。使用实时PCR,在剂量率超过5 cGy/h的低剂量率照射下,观察到Ccng1/细胞周期蛋白G1、Mdm2和Cdkn1A/p21的表达显著升高。这三个Trp53介导的基因也观察到剂量率依赖性。γ射线高剂量率下Ccng1/细胞周期蛋白G1的表达高于低剂量率。然而,低剂量率γ射线的Mdm2表达高于高剂量率时Mdm2的表达。以0.1 cGy/h和1 cGy/h的低剂量率照射的细胞发生G1期阻滞。此外,在以5 cGy/h和10 cGy/h的低剂量率照射的细胞中观察到G2期生长阻滞,这与Trp53介导的Ccng1/细胞周期蛋白G1上调相关。这些结果表明,细胞对辐射的反应取决于所用剂量率;即,在0.1 - 1 cGy/h剂量率下观察到的反应与在超过5 cGy/h剂量率下观察到的反应不同。

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