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p53靶基因bax、fas、mdm2和waf1/p21在小鼠电离辐射前后的组织和细胞特异性表达。

Tissue and cell-specific expression of the p53-target genes: bax, fas, mdm2 and waf1/p21, before and following ionising irradiation in mice.

作者信息

Bouvard V, Zaitchouk T, Vacher M, Duthu A, Canivet M, Choisy-Rossi C, Nieruchalski M, May E

机构信息

Laboratoire de Cancérogenèse Moléculaire, UMR 217 CEA-CNRS, DRR, DSV, Centre d'Etude Nucleaire, Fontenay aux Roses, France.

出版信息

Oncogene. 2000 Feb 3;19(5):649-60. doi: 10.1038/sj.onc.1203366.

Abstract

The mechanisms by which the p53 tumour suppressor protein would, in vivo, co-ordinate the adaptive response to genotoxic stress is poorly understood. p53 has been shown to transactivate several genes that could be involved in two main cellular responses, growth arrest and apoptosis. To get further insight into the tissue-specific regulation of p53 transcriptional activity, we performed an extensive study looking at the expression of four well characterized p53-responsive genes, before and after gamma-irradiation in p53 wild-type (p53+/+) and p53-deficient (p53-/-) mice. The waf1, bax, fas and mdm2 genes were chosen for their different potential roles in the cellular response to stress. Our data demonstrate the strict p53-dependence of mRNA up-regulation for bax, fas and mdm2 in irradiated tissues and confirm such findings for waf1. They further highlight complex levels of regulatory mechanisms that could lead, in vivo, to selective transcriptional activation of genes by p53. In addition, our results provide arguments for the involvement of p53 in the basal mRNA expression of the four genes in some organs. Finally, in situ expression of Bax and p21Waf-1 protein suggests, at least in lymphoid organs, a direct correlation between selective p53-target gene expression and a particular response of a cell to ionising radiation.

摘要

目前人们对p53肿瘤抑制蛋白在体内协调对基因毒性应激的适应性反应的机制了解甚少。p53已被证明可反式激活多个可能参与两种主要细胞反应(生长停滞和凋亡)的基因。为了更深入了解p53转录活性的组织特异性调控,我们进行了一项广泛的研究,观察了p53野生型(p53+/+)和p53缺陷型(p53-/-)小鼠在γ射线照射前后四个特征明确的p53反应性基因的表达情况。选择waf1、bax、fas和mdm2基因是因为它们在细胞应激反应中具有不同的潜在作用。我们的数据证明了受照射组织中bax、fas和mdm2的mRNA上调严格依赖于p53,并证实了waf1的相关发现。这些数据进一步突出了复杂的调控机制水平,这些机制在体内可能导致p53对基因的选择性转录激活。此外,我们的结果为p53参与某些器官中这四个基因的基础mRNA表达提供了依据。最后,Bax和p21Waf-1蛋白的原位表达表明,至少在淋巴器官中,p53靶基因的选择性表达与细胞对电离辐射的特定反应之间存在直接关联。

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