Poor clinical significance of p53 gene polymorphism in acute myeloid leukemia

Abstract 

The cancer susceptibility according to the p53 polymorphism at codon 72 has been in controversy. In this study, the clinical significance of p53 polymorphism in de novo acute myeloid leukemia (AML) was examined. Although the allelic frequency of Arg in 200 patients with AML (64.3%) tended to be greater than that in normal controls (56.6%), these frequencies were within the normal range according to the previous data in Japan (from 59.9 to 65.3%). p53 mutations, found in nine (4.5%) of the 200 patients, were not related to the polymorphism. Six of 93 patients showing heterozygosity at codon 72 had allelic imbalance according to the polymerase chain reaction assay, which occurred in either allele and was associated with p53 mutation and poor prognosis (P=0.01). However, the p53 polymorphism was not associated with clinical features, complete remission rates or prognosis of AML. These results indicate that the p53 genotype at codon 72 is useful to detect loss of heterozygosity but not associated with risk, pathophysiology or therapeutic response of AML.

Keywords:  Acute myeloid leukemia, p53, Polymorphism, Cancer susceptibility, Loss of heterozygosity, Prognosis

Abbreviations:  AML, acute myeloid leukemia, HPV, human papilloma virus, CR, complete remission, OS, overall survival, FAB, French–American–British, PCR, polymerase chain reaction, SSCP, single strand conformation polymorphism, BMT, bone marrow transplantation, LOH, loss of heterozygosity