Modulation of the vitamin D3 response by cancer-associated mutant p53.

癌症相关突变 p53 对维生素 D3 反应的调节

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作者:Stambolsky Perry, Tabach Yuval, Fontemaggi Giulia, Weisz Lilach, Maor-Aloni Revital, Siegfried Zehava, Shiff Idit, Kogan Ira, Shay Moshe, Kalo Eyal, Blandino Giovanni, Simon Itamar, Oren Moshe, Rotter Varda
The p53 gene is mutated in many human tumors. Cells of such tumors often contain abundant mutant p53 (mutp53) protein, which may contribute actively to tumor progression via a gain-of-function mechanism. We applied ChIP-on-chip analysis and identified the vitamin D receptor (VDR) response element as overrepresented in promoter sequences bound by mutp53. We report that mutp53 can interact functionally and physically with VDR. Mutp53 is recruited to VDR-regulated genes and modulates their expression, augmenting the transactivation of some genes and relieving the repression of others. Furthermore, mutp53 increases the nuclear accumulation of VDR. Importantly, mutp53 converts vitamin D into an antiapoptotic agent. Thus, p53 status can determine the biological impact of vitamin D on tumor cells.

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