研究进展, 更新时间: 2005年9月9日
  由美国生科集团 (BVTech, Inc.) 主办
  
肿瘤抑止基因p53的 多种转录方式
2005-9-9
  

Lane研究组首次揭示肿瘤抑止基因p53有多个启动子, 从而可转录出六种蛋白.这些蛋白质(isoform)的表达在不同组织之间存在差异. 更重要的是,它们的表达在癌变时发生变化. 据此推测, 这些 isoform可能互相作用进而调控下游基因表达.


p53 isoforms can regulate p53 transcriptional activity

Jean-Christophe Bourdon3, Kenneth Fernandes, Fiona Murray-Zmijewski, Geng Liu, Alexandra Diot, Dimitris P. Xirodimas, Mark K. Saville and David P. Lane1,2

The recently discovered p53-related genes, p73 and p63, express multiple splice variants and N-terminally truncated forms initiated from an alternative promoter in intron 3. To date, no alternative promoter and multiple splice variants have been described for the p53 gene. In this study, we show that p53 has a gene structure similar to the p73 and p63 genes. The human p53 gene contains an alternative promoter and transcribes multiple splice variants. We show that p53 variants are expressed in normal human tissue in a tissue-dependent manner. We determine that the alternative promoter is conserved through evolution from Drosophila to man, suggesting that the p53 family gene structure plays an essential role in the multiple activities of the p53 family members. Consistent with this hypothesis, p53 variants are differentially expressed in human breast tumors compared with normal breast tissue. We establish that p53 can bind differentially to promoters and can enhance p53 target gene expression in a promoter-dependent manner, while 133p53 is dominant-negative toward full-length p53, inhibiting p53-mediated apoptosis. The differential expression of the p53 isoforms in human tumors may explain the difficulties in linking p53 status to the biological properties and drug sensitivity of human cancer.

Sourec:Genes Dev. Doi: 10.1101/gad.1339905 (2005)


 

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