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TP53 codon 72 polymorphism and cervical cancer

Authors :: R.J. Pegoraro
Annarosa Del Mistro
M. Pillai
Dhananjaya Saranath
Angel Suarez-Rincon
Joseph Menczer
Adam N. Rosenthal
Giovanni Rezza
Åslaug Helland
Theodoros Agorastos
Virginia M. Schmitt
Maria Blettner
Mark H. Stoler
Jae Weon Kim
Stefanie J. Klug
Ming-Tsang Wu
Sylvia M. F. Brenna
Margaret M. Madeleine
Andrea L. Haws
Peter J.F. Snijders
Wannapa Settheetham-Ishida
Meike Ressing
Martín Carlos Abba
Aleksandra Dybikowska
Marco Ciotti
Tsuyoshi Yamashita
Masatsugu Ueda
Gulielmina Ranzani
Magnus von Knebel Doeberitz
Zivile Gudleviciene
Sun H. Jee
Alan Hildesheim
Hextan Y.S. Ngan
Ate G.J. van der Zee
Krisztina Szarka
Sharmila Sengupta
Ulf Gyllensten
Anna R. Giuliano
Yoshimitsu Niwa
Hiroshi Shirasawa
Ruth Tachezy
Susanta Roychoudhury
Olivier Humbey
Akira Nishikawa
C. Simon Herrington
Ingeborg Zehbe
Jochem Koenig
B. R. Das
Carcinogénèse épithéliale : facteurs prédictifs et pronostiques - UFC ( CEF2P / CARCINO )
Centre Hospitalier Régional Universitaire [Besançon] ( CHRU Besançon ) -Université Bourgogne Franche-Comté ( UBFC ) -Université de Franche-Comté ( UFC )
Targeted Gynaecologic Oncology (TARGON)
Carcinogénèse épithéliale : facteurs prédictifs et pronostiques - UFC (EA 3181) (CEF2P / CARCINO)
Université de Franche-Comté (UFC)
Université Bourgogne Franche-Comté [COMUE] (UBFC)-Université Bourgogne Franche-Comté [COMUE] (UBFC)-Centre Hospitalier Régional Universitaire de Besançon (CHRU Besançon)
Pathology
CCA - Oncogenesis
Source :: Lancet Oncology, Lancet Oncology, Elsevier, 2009, 10 (8), pp.772-784. 〈10.1016/S1470-2045(09)70187-1〉, Lancet Oncology, 10(8), 772-784. ELSEVIER SCIENCE INC, Klug, S J, Ressing, M E, Koenig, J, Abba, M C, Agorastos, T, Brenna, S M F, Ciotti, M, Das, B R, Del Mistro, A, Dybikowska, A, Giuliano, A R, Gudleviciene, Z, Gyllensten, U, Haws, A L F, Helland, A, Herrington, C S, Hildesheim, A, Humbey, O, Jee, S H, Kim, J T, Madeleine, M M, Menczer, J, Ngan, H Y S, Nishikawa, A, Niwa, Y, Pegoraro, R, Pillai, M R, Ranzani, G, Rezza, G, Rosenthal, A J, Roychoudhury, S, Saranath, D, Schmitt, V M, Sengupta, S, Settheetham-Ishida, W, Shirasawa, H, Snijders, P J F, Stoler, M H, Suarez-Rincon, A E, Szarka, K, Tachezy, R, Ueda, M, van der Zee, A, Doeberitz, M, Wu, M, Yamashita, T, Zehbe, I & Blettner, M 2009, ' TP53 codon 72 polymorphism and cervical cancer: a pooled analysis of individual data from 49 studies ', Lancet Oncology, vol. 10, no. 8, pp. 772-784 . https://doi.org/10.1016/S1470-2045(09)70187-1, Lancet Oncology, Elsevier, 2009, 10 (8), pp.772-784. ⟨10.1016/S1470-2045(09)70187-1⟩, Lancet Oncology, 10(8), 772-784. Lancet Publishing Group
Publication Year :: 2009
Publisher :: ELSEVIER SCIENCE INC, 2009.
Abstract: Background Cervical cancer is caused primarily by human papillomaviruses (HPV). The polymorphism rs1042522 at codon 72 of the TP53 tumour-suppressor gene has been investigated as a genetic cofactor. More than 80 studies were done between 1998 and 2006, after it was initially reported that women who are homozygous for the arginine allele had a risk for cervical cancer seven times higher than women who were heterozygous for the allele. However, results have been inconsistent. Here we analyse pooled data from 49 studies to determine whether there is an association between TP53 codon 72 polymorphism and cervical cancer.Methods Individual data on 7946 cases and 7888 controls from 49 different studies worldwide were reanalysed. Odds ratios (OR) were estimated using logistic regression, stratifying by study and ethnic origin. Subgroup analyses were done for infection with HPV, ethnic origin, Hardy-Weinberg equilibrium, study quality, and the material used to determine TP53 genotype.Findings The pooled estimates (OR) for invasive cervical cancer were 1.22 (95% CI 1.08-1-39) for arginine homozygotes compared with heterozygotes, and 1.13 (0.94-1.35) for arginine homozygotes versus proline homozygotes. Subgroup analyses showed significant excess risks only in studies where controls were not in Hardy-Weinberg equilibrium (1.71 [1.21-2.42] for arginine homozygotes compared with heterozygotes), in non-epidemiological studies (1.35 [1.15-1.58] for arginine homozygotes compared with heterozygotes), and in studies where TP53 genotype was determined from tumour tissue (1.39 [1.13-1.73] for arginine homozygotes compared with heterozygotes). Null results were noted in studies with sound epidemiological design and conduct (1.06 [0.87-1.29] for arginine homozygotes compared with heterozygotes), and studies in which TP53 genotype was determined from white blood cells (1.06 [0.87-1.29] for arginine homozygotes compared with heterozygotes).Interpretation Subgroup analyses indicated that excess risks were most likely not due to clinical or biological factors, but to errors in study methods. No association was found between cervical cancer and TP53 codon 72 polymorphism when the analysis was restricted to methodologically sound studies.Funding German Research Foundation (DFG).