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Rescue of early embryonic lethality in mdm2-deficient mice by deletion of p53

Nature volume 378pages 203–206 (1995)Cite this article

Abstract

THE gene p53 encodes a transcriptional activator1,2 of genes involved in growth arrest3,4, DNA repair5 and apoptosis6–8. Loss of p53 function contributes to tumour development in vivo 9–11. The transcriptional activation function of p53 is inactivated by interaction with the mdnil gene product12–14. Amplification of mdm2 has been observed in 36% of human sarcomas, indicating that it may represent an alternative mechanism of preventing p53 function in tumour development15. To study mdm2 function in vivo, we generated an mdm2 null allele by homologous recombination. Mdm2 null mice are not viable, and further analysis revealed embryonic lethality around implantation. To examine the importance of the interaction of MDM2 with p53 in vivo, we crossed mice heterozygous for mdm2 and p53 and obtained progeny homozygous for both p53 and mdm2 null alleles. Rescue of the mdm2/ lethality in a p53 null background suggests that a critical in vivo function of MDM2 is the negative regulation of p53 activity.

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Authors and Affiliations

  1. Department of Molecular Genetics, University of Texas, M.D. Anderson Cancer Center, 1515 Holcombe Boulevard, Houston, Texas, 77030, USA

    Roberta Montes de Oca Luna & Guillermina Lozano

  2. Department of Biochemistry and Molecular Biology, University of Texas, M.D. Anderson Cancer Center, 1515 Holcombe Boulevard, Houston, Texas, 77030, USA

    Daniel S. Wagner

Authors
  1. Roberta Montes de Oca Luna
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  2. Daniel S. Wagner
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  3. Guillermina Lozano
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de Oca Luna, R., Wagner, D. & Lozano, G. Rescue of early embryonic lethality in mdm2-deficient mice by deletion of p53. Nature 378, 203–206 (1995). https://doi.org/10.1038/378203a0

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