| Literature DB >> 33594052 |
Arvind Singh Mer1,2,3, Emily M Heath1, Seyed Ali Madani Tonekaboni1,2, Nergiz Dogan-Artun1, Sisira Kadambat Nair1, Alex Murison1, Laura Garcia-Prat1, Liran Shlush4, Rose Hurren1, Veronique Voisin5, Gary D Bader5,6, Corey Nislow7, Mattias Rantalainen3, Soren Lehmann3, Mark Gower8, Cynthia J Guidos8, Mathieu Lupien1,2,9, John E Dick1,10, Mark D Minden1, Aaron D Schimmer11, Benjamin Haibe-Kains12,13,14,15,16.
Abstract
In acute myeloid leukemia (AML), molecular heterogeneity across patients constitutes a major challenge for prognosis and therapy. AML with NPM1 mutation is a distinct genetic entity in the revised World Health Organization classification. However, differing patterns of co-mutation and response to therapy within this group necessitate further stratification. Here we report two distinct subtypes within NPM1 mutated AML patients, which we label as primitive and committed based on the respective presence or absence of a stem cell signature. Using gene expression (RNA-seq), epigenomic (ATAC-seq) and immunophenotyping (CyToF) analysis, we associate each subtype with specific molecular characteristics, disease differentiation state and patient survival. Using ex vivo drug sensitivity profiling, we show a differential drug response of the subtypes to specific kinase inhibitors, irrespective of the FLT3-ITD status. Differential drug responses of the primitive and committed subtype are validated in an independent AML cohort. Our results highlight heterogeneity among NPM1 mutated AML patient samples based on stemness and suggest that the addition of kinase inhibitors to the treatment of cases with the primitive signature, lacking FLT3-ITD, could have therapeutic benefit.Entities:
Year: 2021 PMID: 33594052 DOI: 10.1038/s41467-021-21233-0
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919