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Distinct association between aberrant methylation of Wnt inhibitors and genetic alterations in acute myeloid leukaemia
Journal
British Journal of Cancer
Journal Volume
105
Journal Issue
12
Pages
1927-1933
Date Issued
2011
Author(s)
Kuo Y.-Y.
Liu C.-Y.
Lee M.C.
Huang C.-F.
Lee F.-Y.
Liu M.-C.
Abstract
Background: Aberrant activation of Wnt signalling through hypermethylation of Wnt inhibitor genes is involved in several human malignancies, including acute myeloid leukaemia (AML). It remains unclear whether hypermethylation of Wnt inhibitors is associated with molecular gene mutations in the development of AML. Methods: We investigated the association of the promoter hypermethylation of six Wnt inhibitors (Wif-1, SFRP1, SFRR2, SFRP4, SFRP5, and DKK1) with gene aberrations in the leukaemogenesis of 269 AML patients. Results: In total, 166 patients (61.7%) had hypermethylation of at least one Wnt inhibitor. The majority (68.5%) of patients with Wnt inhibitor hypermethylation had concurrent Class II gene mutations that affect transcription factors or cofactors. There was a close association of Wif-1 hypermethylation with t(15;17) (P0.0005) and CEBPA mutation (P0.0001), DKK1 hypermethylation with t(8;21) (P0.0001) and ASXL1 mutation (P0.0078), SFRP-1 hypermethylation with t(8;21) (P0.0001), SFRP-2 hypermethylation with AML1/RUNX1 mutation (P0.0012), and SFRP-5 hypermethylation with MLL/PTD (P0.0505). On the other side, hypermethylation of Wnt inhibitors was always negatively associated with NPM1 mutation and FLT3/ITD. Conclusion: There was distinct association between hypermethylation of individual Wnt inhibitors and specific gene aberrations, especially Class II mutations. The Wnt inhibitor hypermethylation might interact with genetic alterations in the leukaemogenesis. ? 2011 Cancer Research UK All rights reserved.
SDGs
Other Subjects
CD11b antigen; CD135 antigen; CD14 antigen; CD19 antigen; CD34 antigen; CD7 antigen; dickkopf 1 protein; HLA DR antigen; lactate dehydrogenase; nucleophosmin; protein inhibitor; secreted frizzled related protein 1; secreted frizzled related protein 2; secreted frizzled related protein 4; secreted frizzled related protein 5; transcription factor RUNX1; unclassified drug; Wnt inhibitory factor 1; Wnt protein; Wnt protein; acute granulocytic leukemia; adolescent; adult; aged; antigen expression; article; controlled study; cytogenetics; female; gene mutation; genetic association; human; human cell; immunophenotyping; lactate dehydrogenase blood level; leukemogenesis; leukocyte count; major clinical study; male; priority journal; promoter region; protein methylation; sex difference; thrombocyte count; treatment response; DNA methylation; drug antagonism; genetics; immunology; mutation; pathology; polymerase chain reaction; Adult; DNA Methylation; Humans; Immunophenotyping; Leukemia, Myeloid, Acute; Mutation; Polymerase Chain Reaction; Wnt Proteins
Type
journal article