Centre for Oncology and Molecular Medicine, INSERM-European Associated Laboratory, Ninewells Hospital and Medical School, Dundee, DD1 9SY, Scotland, UK.
Cell Death Differ. 2012 May;19(5):816-26. doi: 10.1038/cdd.2011.152. Epub 2011 Nov 11.
In response to stress, p53 binds and transactivates the internal TP53 promoter, thus regulating the expression of its own isoform, Δ133p53α. Here, we report that, in addition to p53, at least four p63/p73 isoforms regulate Δ133p53 expression at transcriptional level: p63β, ΔNp63α, ΔNp63β and ΔNp73γ. This regulation occurs through direct DNA-binding to the internal TP53 promoter as demonstrated by chromatin immunoprecipitation and the use of DNA-binding mutant p63. The promoter regions involved in the p63/p73-mediated transactivation were identified using deleted, mutant and polymorphic luciferase reporter constructs. In addition, we observed that transient expression of p53 family members modulates endogenous Δ133p53α expression at both mRNA and protein levels. We also report concomitant variation of p63 and Δ133p53 expression during keratinocyte differentiation of HaCat cells and induced pluripotent stem cells derived from mutated p63 ectodermal dysplasia patients. Finally, proliferation assays indicated that Δ133p53α isoform regulates the anti-proliferative activities of p63β, ΔNp63α, ΔNp63β and ΔNp73γ. Overall, this study shows a strong interplay between p53, p63 and p73 isoforms to orchestrate cell fate outcome.
在应对压力时,p53 结合并反式激活内部 TP53 启动子,从而调节其自身异构体 Δ133p53α 的表达。在这里,我们报告说,除了 p53 之外,至少有四种 p63/p73 异构体通过直接与内部 TP53 启动子结合在转录水平上调节 Δ133p53 的表达:p63β、ΔNp63α、ΔNp63β 和 ΔNp73γ。这一调节作用是通过染色质免疫沉淀和使用 DNA 结合突变体 p63 来证明的。使用缺失、突变和多态性荧光素酶报告构建体鉴定了涉及 p63/p73 介导的反式激活的启动子区域。此外,我们观察到 p53 家族成员的瞬时表达在 mRNA 和蛋白水平上均调节内源性 Δ133p53α 的表达。我们还报告了 HaCat 细胞角质形成细胞分化和突变型 p63 外胚层发育不良患者来源的诱导多能干细胞中 p63 和 Δ133p53 的表达同时发生变化。最后,增殖测定表明 Δ133p53α 异构体调节 p63β、ΔNp63α、ΔNp63β 和 ΔNp73γ 的抗增殖活性。总体而言,这项研究表明 p53、p63 和 p73 异构体之间存在强烈的相互作用,以协调细胞命运的结果。
