Distinct karyotypic and mutational landscape in trisomy AML.

Stephen S Y LamSze P TsuiC Y FungNicole Y SawAsif JavedAlvin H W IpEdmond Shiu-Kwan Ma Anskar Yu-Hung Leung

Published in: British journal of haematology (2023)

Trisomy karyotype occurs in 5%-10% of AML. Its mutational landscape and prognostic significance are not well defined. A cohort of 156 trisomy AML patients was analysed, with reference to 615 cytogenetically normal (CN) AML patients. Trisomy AML showed distinct mutational landscape with more prevalent SMC1A, N/KRAS, ASXL1 and BCOR but fewer CEBPA bZIP and NPM1 mutations in patients ≤60, and fewer NPM1 mutations in those >60. NRAS mutations were associated with poor outcome in trisomy AML, whereas DNMT3A and FLT3-ITD mutations had neutral effect. Trisomy AML appeared biologically distinct from CN-AML.

Keyphrases

acute myeloid leukemia
end stage renal disease
allogeneic hematopoietic stem cell transplantation
chronic kidney disease
newly diagnosed
prognostic factors
peritoneal dialysis
single cell
dna methylation
patient reported outcomes
transcription factor
patient reported