GSTM1 and GSTP1, but not GSTT1 genetic polymorphisms are associated with chronic myeloid leukemia risk and treatment response

FERRI C; GIERE I; FUNDIA AF; WEICH N; BENGIO R; LARRIPA IB; MOIRAGHI B; PAVLOVSKY C

CANCER EPIDEMIOLOGY

ELSEVIER SCI LTD

Lugar: Amsterdam; Año: 2016

1877-7821

Background: Chronic myeloid leukemia (CML) is associated to the BCR-ABL1 oncogene and can successfully be treated with tyrosine kinase inhibitors (TKIs). However, it remains still under investigation which molecular factors may influence CML risk or varying responses to TKIs. The aim of this study was to assess the role of Glutathione-S- transferases (GSTs) genetic polymorphisms in CML susceptibility and TKI clinical outcome.Materials: Deletion polymorphisms in GSTM1 and GSTT1 genes and the single nucleotide polymorphism in GSTP1 c.319A>G (rs1695; p.105Ile>Val) were genotyped by PCR methods in 141 CML treated patients and 141 sex- and age-matched healthy individualsResults: Individual analysis of each GST gene showed no association with CML risk. A trend toward significance (p=0.07) for a recessive model was found for GSTP1 (OR: 2.04; IC: 0.94-4.4). However, the combined analysis showed that GSTM1-null/GSTP1- GG as well as GSTT1-null/GSTP1- GG were associated with CML development (p= 0.03; OR: 3.54 IC: 1.2-14.57; p= 0.05; OR: 12.65; IC: 1.17-21.5). The relationship with treatment outcome showed that the presence of GSTM1 gene was significantly linked with an inferior rate of major molecular response (p=0.048) and poor event free-survival (EFS)(p=0.02).Furthermore, a group of patients with GSTP1-GG genotype were significantly associated with reduced EFS comparing to those carrying other GSTP1 genotypes (p=0.049). GSTP1-GG genotypes had short time to treatment failure in a group of patients unresponsive to TKIs comparing to other GSTP1 genotypes (p=0.03).Conclusions: This study highlights the significance of GSTs polymorphisms on CML susceptibility and response to TKIs in the Argentinean population.