Journal
JOURNAL OF BIOLOGICAL CHEMISTRY
Volume 282, Issue 25, Pages 18365-18378Publisher
AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.M610522200
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In response to DNA damage, p53 and its homolog p73 have a function antagonistic to NF-kappa B in deciding cell fate. Here, we show for the first time that p73, but not p53, is stabilized by physical interaction with nuclear I kappa B kinase (IKK)-alpha to enhance cisplatin (CDDP)-induced apoptosis. CDDP caused a significant increase in the amounts of nuclear IKK-alpha and p73 alpha in human osteosarcoma-derived U2OS cells. Ectopic expression of IKK-alpha prolonged the half-life of p73 by inhibiting its ubiquitination and thereby enhancing its transactivation and pro-apoptotic activities. Consistent with these results, small interfering RNA-mediated knockdown of endogenous IKK-alpha inhibited the CDDP-mediated accumulation of p73 alpha. The kinase-deficient mutant form of IKK-alpha interacted with p73 alpha, but failed to stabilize it. Furthermore, CDDP-mediated accumulation of endogenous p73 alpha was not detected in mouse embryonic fibroblasts (MEFs) prepared from IKK-alpha-deficient mice, and CDDP sensitivity was significantly decreased in IKK-alpha-deficient MEFs compared with wild-type MEFs. Thus, our results strongly suggest that the nuclear IKK-alpha-mediated accumulation of p73 alpha is one of the novel molecular mechanisms to induce apoptotic cell death in response to CDDP, which may be particularly important in killing tumor cells with p53 mutation.
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