Abstract
p73, a novel p53 family member, is a recently identified candidate neuroblastoma (NBL) suppressor gene mapped at chromosome 1p36.33 and was found to inhibit growth and induce apoptosis in cell lines. To test the hypothesis that p73 is a NBL suppressor gene, we analysed the p73 gene in primary human NBLs. Loss of heterozygosity (LOH) for p73 was observed in 19% (28/151) of informative cases which included 92 mass-screening (MS) tumors. The high frequency of p73 LOH was significantly associated with sporadic NBLs (9% vs 34%, P<0.001), N-myc amplification (10% vs 71%, P<0.001), and advanced stage (14% vs 28%, P<0.05). Both p73α and p73β transcripts were detectable in only 46 of 134 (34%) NBLs at low levels by RT – PCR methods, while they were easily detectable in most breast cancers and colorectal cancers under the same conditions. They found no correlation between p73 LOH and its expression levels (P>0.1). We found two mutations out of 140 NBLs, one somatic and one germline, which result in amino acid substitutions in the C-terminal region of p73 which may affect transactivation functions, though, in the same tumor samples, no mutation of the p53 gene was observed as reported previously. These results suggest that allelic loss of the p73 gene may be a later event in NBL tumorigenesis. However, p73 is infrequently mutated in primary NBLs and may hardly function as a tumor suppressor in a classic Knudson's manner.
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References
Amler LC, Corvi R, Praml C, Savelyeva L, Le Paslier D and Schwab M. . 1995 Oncogene 10: 1095–1101.
Brodeur GM, Pritchard J, Berthold F, Carlsen NL, Castel V, Castelberry RP, De Bernardi B, Evans AE, Favrot M, Hedborg F, Kaneko M, Kemshead J, Lampert F, Lee REJ, Look T, Pearson ADJ, Philip T, Roald B, Sawada T, Seeger RC, Tsuchida Y and Voute PA. . 1993 J. Clin. Oncol. 11: 1466–1477.
Caron H, Peter M, van Sluis P, Speleman F, de Kraker J, Laureys G, Michon J, Brugieres L, Voute PA, Westerveld A, Slater R, Delattre O and Versteeg R. . 1995 Hum. Mol. Genet. 4: 535–539.
Cheng JM, Hiemstra JL, Schneider SS, Naumova A, Cheung NK, Cohn SL, Diller L, Sapienza C and Brodeur GM. . 1993 Nature Genet. 4: 191–194.
Christiansen H, Schestag J, Christiansen NM, Grzeschik K and Lampert F. . 1992 Genes Chromosom. Cancer 5: 141–149.
Fong CT, White PS, Peterson K, Sapienza C, Cavenee WK, Kern SE, Vogelstein B, Cantor AB, Look AT and Brodeur GM. . 1992 Cancer Res. 52: 1780–1785.
Jost CA, Marin MC and Kaelin Jr WG. . 1997 Nature 389: 191–194.
Kaghad M, Bonnet H, Yang A, Creancier L, Biscan JC, Valent A, Minty A, Chalon P, Lelias JM, Dumont X, Ferrara P, McKeon F and Caput D. . 1997 Cell 90: 809–819.
Kobayashi H, Satake N, Maseki N, Sakashita A and Kaneko Y. . 1996 Br. J. Haematol. 94: 105–111.
Komuro H, Hayashi Y, Kawamura M, Hayashi K, Kaneko Y, Kamoshita S, Hanada R, Yamamoto K, Hongo T, Yamada M and Tsuchida Y. . 1993 Cancer Res. 53: 5284–5288.
Mai M, Yokomizo A, Qian C, Yang P, Tindall DJ, Smith DI and Liu W. . 1998 Cancer Res. 58: 2347–2349.
Martinsson T, Sjoberg R-M, Hedborg F and Kogner P. . 1995 Cancer Res. 55: 5681–5686.
Mashiyama S, Murakami Y, Yoshimoto T, Sekiya T and Hayashi K. . 1991 Oncogene 6: 1313–1318.
Mihara M, Nimura Y, Ichimiya S, Sakiyama S, Kajikawa S, Adachi W, Amano J and Nakagawara A. . 1998 Br. J. Cancer in press.
Moll UM, LaQuaglia M, Benard J and Riou G. . 1995 Proc. Natl. Acad. Sci. USA 92: 4407–4411.
Nakagawara A, Arima-Nakagawara M, Scavarda NJ, Azar CG, Cantor A and Brodeur GM. . 1993 N. Engl. J. Med. 328: 847–854.
Nakagawara A, Arima M, Azar CG, Scavarda NJ and Brodeur GM. . 1992 Cancer Res. 52: 1364–1368.
Nakagawara A, Azar CG, Scavarda NJ and Brodeur GM. . 1994 Mol. Cell. Biol. 14: 759–767.
Nimura Y, Mihara M, Ichimiya S, Sakiyama S, Seki N, Ohira M, Nomura N, Fujimori M, Adachi W, Amano J, He M, Ping Y-M and Nakagawara A. . 1998 Int. J. Cancer in press.
Nomoto S, Haruki N, Kondo M, Konishi H, Takahashi T, Takahashi T and Takahashi T. . 1998 Cancer Res. 58: 1380–1383.
Ohira M, Ichikawa H, Suzuki E, Iwaki M, Suzuki K, Saito-Ohara F, Ikeuchi T, Chumakov I, Tanahashi H, Tashiro K, Sakaki Y and Ohki M. . 1996 Genomics 33: 65–74.
Ohtsu K, Hiyama E, Ichikawa T, Matsuura Y and Yokoyama T. . 1997 Clin. Cancer Res. 3: 1221–1228.
Ostermeyer AG, Runko E, Winkfield B, Ahn B and Moll UM. . 1996 Proc. Natl. Acad. Sci. USA 93: 15190–15194.
Schleiermacher G, Peter M, Michon J, Hugot JP, Vielh P, Zucker JM, Magdelenat H, Thomas G and Delattre O. . 1994 Genes Chromosomes Cancer 10: 275–281.
Schwab M, Praml C and Amler LC. . 1996 Genes Chrom. Cancer 16: 211–229.
Shepherd NS, Pfrogner BD, Coulby JN, Ackerman SL, Vaidyanathan G, Sauer RH, Balkenhol TC and Sternberg N. . 1994 Proc. Natl. Acad. Sci. USA 91: 2629–2633.
Sunahara M, Ichimiya S, Nimura Y, Takada N, Sakiyama S, Sato Y, Todo S, Adachi W, Amano J and Nakagawara A. . 1998 Int. J. Oncol. 13: 319–323.
Takahashi H, Ichimiya S, Nimura Y, Watanabe M, Furusato M, Wakui S, Yatani R, Aizawa S and Nakagawara A. . 1998 Cancer Res. 58: 2076–2077.
Takeda O, Homma C, Maseki N, Sakurai M, Kanda N, Schwab M, Nakamura Y and Kaneko Y. . 1994 Genes Chromosomes Cancer 10: 30–39.
Vogan K, Bernstein M, Leclerc JM, Brisson L, Brossard J, Brodeur GM, Pelletier J and Gros P. . 1993 Cancer Res. 53: 5269–5273.
White PS, Maris JM, Beltinger C, Sulman E, Marshall HN, Fujimori M, Kaufman BA, Biegel JA, Allen C, Hilliard C, Valentine MB, Look AT, Enomoto H, Sakiyama S and Brodeur GM. . 1995 Proc. Natl. Acad. Sci. USA 92: 5520–5524.
Acknowledgements
The authors thank Eiji Hanaoka for experimental support, and Makoto Kasama, Aiko Morohashi and Naoko Sugimitsu for technical assistance. The authors also thank the following institutes for providing surgical samples and clinical data: First Department of Surgery, Hokkaido University; Department of Pediatrics, National Sapporo Hospital; Department of Pediatric Surgery, Tohoku University; Department of Pediatric Surgery, Iwate Prefectural Central Hospital; Department of Surgery, Gunma Children's Medical Center; Department of Pediatric Surgery, Jichi Medical University; Department of Hematology and Oncology, Saitama Children's Medical Center; Department of Pediatric Surgery, Tsukuba University; Department of Pediatrics, Juntendo University; Department of Surgery, Kiyose Metropolitan Children's Hospital; Departments of Surgery and Pathology, Chiba Children's Hospital; Department of Pediatric Surgery, Matsudo Municipal Hospital; Department of Pediatric Surgery, Chiba University; Department of Pediatric Surgery, Kimitsu Central Hospital; Department of Pediatric Surgery, Niigata University; Department of Pediatric Surgery, Niigata Municipal Hospital; Department of Pediatrics, Aichi Medical University; Department of Pediatrics, Kyoto Prefectural Medical University; Department of Pediatric Surgery, Osaka City General Medical Center; Department of Pediatrics, Osaka Medical University; Tumor Board, Hyogo Children's Hospital; Department of Pediatric Surgery, Kumamoto University; Departments of Pediatrics and Pediatric Surgery, Kagoshima University. This work was supported in part by a grant-in-aid from the Ministry of Health and Welfare for a New Comprehensive 10-Year Strategy for Cancer Control, Japan, a grant from the Naito Foundation, and a grant from the Japanese Foundation for Multidisciplinary Treatment of Cancer. S.I. is an awardee of Research Resident Fellowship from the Foundation for the Promotion of Cancer Research.
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Ichimiya, S., Nimura, Y., Kageyama, H. et al. p73 at chromosome 1p36.3 is lost in advanced stage neuroblastoma but its mutation is infrequent. Oncogene 18, 1061–1066 (1999). https://doi.org/10.1038/sj.onc.1202390
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DOI: https://doi.org/10.1038/sj.onc.1202390
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