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Volume 34, Issue 2, Pages 184-188 (April 2010)


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Haplotype analysis of p53 polymorphisms: Arg72Pro, Ins16bp and G13964C in Tunisian patients with familial or sporadic breast cancer

Fatma Trifaa, Sondes Karray-Chouayekha, Imed Mabrouka, Sami Baccouchea, Abdelmajid Khabirb, Tahia Sellami-Boudawarab, Ali Gargouria, Raja Mokdad-GargouriaCorresponding Author Informationemail address

Accepted 13 February 2010. published online 02 March 2010.

Abstract 

Background: The p53 polymorphisms have been extensively studied as putative breast cancer susceptibility variants. The present study was undertaken to investigate the association of p53 Arg72Pro, Ins16bp and G13964C polymorphisms and their haplotypes with breast cancer risk in Tunisian women. Methods: Genotyping was performed by polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) on 159 patients and 132 controls. Results: The G13964C intronic variant was significantly associated with familial breast cancer risk (p=0.0018) while the genotypic distribution was similar for p53 Arg72Pro and Ins16bp in patients and controls. Moreover, the (NoIns-C), (Arg-C) and (NoIns-Arg-C) haplotypes were significantly associated with familial breast cancer risk (p=0.0021, p=0.0096 and p=0.0084, respectively) while there was a trend of association between the (Ins-Arg) and (Ins-Arg-G) haplotypes and the risk of sporadic breast cancer. Only the G/C genotype as well as the (NoIns-C) haplotype remained significant after correction for multiple testing. Conclusion: Our data revealed an association between the G/C genotype and the (NoIns-C) haplotype and the risk of familial breast cancer in Tunisian women. However, these observations need to be confirmed due to the limited statistical power of our study and the small number of cases.

a Unité de Génétique du cancer et Production de protéines thérapeutiques, Centre de Biotechnologie de Sfax, route Sidi Mansour, BP « 1177 », 3018 Sfax, Tunisia

b Centre Hospitalo-Universitaire Habib Bourguiba, 3000 Sfax, Tunisia

Corresponding Author InformationCorresponding author. Tel.: +216 74 874 449.

PII: S1877-7821(10)00026-3

doi:10.1016/j.canep.2010.02.007


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