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Li X , Dumont P , Della Pietra A , Shetler G , Murphy ME
The codon 47 polymorphism in p53 is functionally significant
Journal of Biological Chemistry. 2005 ;280(25) :24245-24251
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In addition to a common polymorphism at codon 72, the p53 tumor suppressor gene also contains a rare single nucleotide polymorphism at amino acid 47. Wild type p53 encodes proline at this residue, but in <5% of African Americans, this amino acid is serine. Notably, phosphorylation of the adjacent serine 46 by the proline-directed kinase p38 MAPK is known to greatly enhance the ability of p53 to induce apoptosis. Here we showed that the serine 47 polymorphic variant, which replaces the proline residue necessary for recognition by proline-directed kinases, is a markedly poorer substrate for phosphorylation on serine 46 by p38 MAPK. Consistent with this finding, we showed that the serine 47 variant has up to 5-fold decreased ability to induce apoptosis compared with wild type p53. Mechanistically, we found that this variant has decreased ability to transactivate two p53 target genes, p53AIP1 and PUMA, but not other p53 response genes; this is the first time that phosphorylation of serine 46 has been implicated in transactivation of PUMA by p53. Down-regulation of PUMA in cells with wild type p53 using short interfering RNAs reduced apoptosis in these cells to a level comparable to that in cells containing the serine 47 variant. The combined data indicated that, like the codon 72 polymorphism, the codon 47 polymorphism of p53 is functionally significant and may play a role in cancer risk, progression, and the efficacy of therapy. © 2005 by The American Society for Biochemistry and Molecular Biology, Inc.
00219258 (ISSN) Cited By: 5; Export Date: 25 May 2006; Source: Scopus CODEN: JBCHA; DOI: 10.1074/jbc.M414637200 Language of Original Document: English Correspondence Address: Murphy, M.E.; Cell and Developmental Biology Program; Fox Chase Cancer Center; 333 Cottman Ave. Philadelphia, PA 19111, United States; email: Maureen.Murphy@FCCC.edu Chemicals/CAS: amino acid, 65072-01-7; proline, 147-85-3, 7005-20-1; serine, 56-45-1, 6898-95-9 References: Dumont, P., Leu, J.I., Della Pietra, A.C., George, D.L., Murphy, M., (2003) Nat. Genet., 33, pp. 357-365; Leu, J.I., Dumont, P., Hafey, M., Murphy, M.E., George, D.L., (2004) Nat. Cell Biol., 6, pp. 443-450; Hishida, A., Matsuo, K., Tajima, K., Ogura, M., Kagami, Y., Taji, H., Morishima, Y., (...), Hamajima, N., (2004) Leuk. Lymphoma, 45, pp. 957-964; Xi, Y.G., Ding, K.Y., Su, X.L., Chen, D.F., You, W.C., Shen, Y., Ke, Y., (2004) Carcinogenesis, 25, pp. 2201-2206; Granja, F., Morari, J., Morari, E.C., Correa, L.A., Assumpcao, L.V., Ward, L.S., (2004) Cancer Lett., 210, pp. 151-157; Jones, J.S., Chi, X., Gu, X., Lynch, P.M., Amos, C.I., Frazier, M.L., (2004) Clin. Cancer Res., 10, pp. 5845-5849; Bond, G.L., Hu, W., Bond, E.E., Robins, H., Lutzker, S.G., Arva, N.C., Bargonetti, J., (...), Levine, A.J., (2004) Cell, 119, pp. 591-602; Felley-Bosco, E., Weston, A., Cawley, H.M., Bennett, W.P., Harris, C.C., (1993) Am. J. Hum. Genet., 53, pp. 752-759; Bulavin, D.V., Saito, S., Hollander, M.C., Sakaguchi, K., Anderson, C.W., Appella, E., Fornace Jr., A.J., (1999) EMBO J., 18, pp. 6845-6854; Oda, K., Arakawa, H., Tanaka, T., Matsuda, K., Tanikawa, C., Mori, T., Nishimori, H., (...), Taya, Y., (2000) Cell, 102, pp. 849-862; Sanchez-Prieto, R., Rojas, J.M., Taya, Y., Gutkind, J.S., (2000) Cancer Res., 60, pp. 2462-2472; Takekawa, M., Adachi, M., Nakahata, A., Nakayama, I., Itoh, F., Tsukuda, H., Taya, Y., Imai, K., (2000) EMBO J., 19, pp. 6517-6526; Bulavin, D.V., Demidov, O.N., Saito, S., Kauraniemi, P., Phillips, C., Amundson, S.A., Ambrosino, C., (...), Appella, E., (2002) Nat. Genet., 31, pp. 210-215; Okamura, S., Arakawa, H., Tanaka, T., Nakanishi, H., Ng, C.C., Taya, Y., Monden, M., Nakamura, Y., (2001) Mol. Cell, 8, pp. 85-94; Pochampally, R., Li, C., Lu, W., Chen, L., Luftig, R., Lin, J., Chen, J., (2000) Biochen. Biophys. Res. Commun., 279, pp. 1001-1010; Murphy, M., Ahn, J., Walker, K.K., Hoffman, W.H., Evans, R.E., Levine, A.J., George, D.L., (1999) Genes Dev., 13, pp. 2490-2501; D'Orazi, G., Cecchinelli, B., Bruno, T., Manni, I., Higashimoto, Y., Saito, S., Gostissa, M., (...), Soddu, S., (2002) Nat Cell Biol., 4, pp. 11-19; Saito, S., Yamaguchi, H., Higashimoto, Y., Chao, C., Xu, Y., Fornace, A.J., Appella, E., Anderson, C.W., (2003) J. Biol. Chem., 278, pp. 37536-37544; Hofmann, T.G., Moller, A., Sirma, H., Zentgraf, H., Taya, Y., Droge, W., Will, H., Schmitz, M.L., (2002) Nat. Cell Biol., 4, pp. 1-10; Martinez, J., Georgoff, I., Martinez, J., Levine, A.J., (1991) Genes Dev., 5, pp. 151-159; Yu, J., Zhang, L., Hwang, P.M., Kinzler, K.W., Vogelstein, B., (2001) Mol. Cell, 7, pp. 673-682; Villunger, A., Michalak, E.M., Coultas, L., Mullauer, F., Bock, G., Ausserlechner, M.J., Adams, J.M., Strasser, A., (2003) Science, 302, pp. 1036-1038; Jeffers, J.R., Parganas, E., Lee, Y., Yang, C., Wang, J., Brennan, J., MacLean, K.H., (...), Zambetti, G.P., (2003) Cancer Cell, 4, pp. 321-328; Olivier, M., Eeles, R., Hollstein, M., Khan, M.A., Harris, C.C., Hainaut, P., (2002) Hum. Mutat., 19, pp. 607-614; McGregor, J.M., Harwood, C.A., Brooks, L., Fisher, S.A., Kelly, D.A., O'Nions, J., Young, A.R., (...), Crook, T., (2002) J. Investig. Dermatol., 119, pp. 84-90; Barak, Y., Gottlieb, E., Juven-Gershon, T., Oren, M., (1994) Genes Dev, 8, pp. 1739-1749.