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• W4361253670 abstract "<div>Abstract<p>The tumor suppressor protein p53 is a transcription factor that induces G₁ arrest of the cell cycle and/or apoptosis. The murine double-minute protein MDM2 and its homologue MDM4 (also known as <i>MDMX</i>) are critical regulators of p53. Altered transcripts of the human homologue of <i>mdm2, MDM2</i>, have been identified in human tumors, such as invasive carcinoma of the breast, lung carcinoma, and liposarcoma. MDM2 alternate forms act to negatively regulate the normal <i>MDM2</i> gene product, thus activating p53. Although many reports have documented a plethora of tumor types characterized by <i>MDM2</i> alternative transcripts, few have investigated the signals that might initiate alternative splicing. We have identified a novel role of these alternative <i>MDM2</i> transcripts in the normal surveillance mechanism of the cell and in DNA damage response. We report that alternate forms of <i>MDM2</i> are detected after UV irradiation. Furthermore, we show that mouse cells treated with UV are also characterized by alternative transcripts of <i>mdm2</i>, suggesting that this is an important and evolutionarily conserved mechanism for regulating the expression of <i>MDM2/mdm2</i>. An additional p53 regulator and <i>mdm2</i> family member, <i>MDM4</i>, is likewise alternatively spliced following UV irradiation. By activating alternative splicing of both <i>MDM2</i> and <i>MDM4</i>, yet another layer of p53 regulation is initiated by the cells in response to damage. A stepwise model for malignant conversion by which alternate forms of MDM2 and MDM4 place selective pressure on the cells to acquire additional alterations in the p53 pathway is herein proposed. (Cancer Res 2006; 66(19): 9502-8)</p></div>" @default.
• W4361253670 created "2023-03-31" @default.
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• W4361253670 date "2023-03-30" @default.
• W4361253670 modified "2023-09-30" @default.
• W4361253670 title "Data from Genotoxic Stress Induces Coordinately Regulated Alternative Splicing of the p53 Modulators MDM2 and MDM4" @default.
• W4361253670 doi "https://doi.org/10.1158/0008-5472.c.6494388.v1" @default.
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