Normal myeloid progenitor cell subset-associated gene signatures for acute myeloid leukaemia subtyping with prognostic impact

Normal myeloid progenitor cell subset-associated gene signatures for acute myeloid leukaemia subtyping with prognostic impact

Acute myeloid leukaemia (AML) is characterised by phenotypic heterogeneity, which we hypothesise is a consequence of deregulated differentiation with transcriptional reminiscence of the normal compartment or cell-of-origin. Here, we propose a classification system based on normal myeloid progenitor...

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Veröffentlicht in:PloS one 2020-04, Vol.15 (4), p.e0229593-e0229593, Article 0229593
Hauptverfasser: Schonherz, Anna A., Bodker, Julie Stove, Schmitz, Alexander, Brondum, Rasmus Froberg, Jakobsen, Lasse Hjort, Roug, Anne Stidsholt, Severinsen, Marianne T., El-Galaly, Tarec C., Jensen, Paw, Johnsen, Hans Erik, Bogsted, Martin, Dybkaer, Karen
Format: Artikel
Sprache:eng
Schlagworte:
Acute myeloid leukemia
Biology and Life Sciences
Bone marrow
Cancer
CD34 antigen
CD38 antigen
CD45RA antigen
Chemotherapy
Classification
Clinical medicine
Cytogenetics
Datasets
Deregulation
Differentiation
Gene expression
Gene set enrichment analysis
Genetics
Genomes
Hematology
Hematopoietic stem cells
Heterogeneity
Immune response
Independent variables
Leukemia
Medical prognosis
Medical research
Medicine
Monocytes
Multidisciplinary Sciences
Mutation
Physical Sciences
Progenitor cells
Quantitative genetics
Regression analysis
Regularization
Research and Analysis Methods
Runx1 protein
Science & Technology
Science & Technology - Other Topics
Signatures
Statistical analysis
Stem cells
Subpopulations
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Zusammenfassung:Acute myeloid leukaemia (AML) is characterised by phenotypic heterogeneity, which we hypothesise is a consequence of deregulated differentiation with transcriptional reminiscence of the normal compartment or cell-of-origin. Here, we propose a classification system based on normal myeloid progenitor cell subset-associated gene signatures (MAGS) for individual assignments of AML subtypes. We generated a MAGS classifier including the progenitor compartments CD34(+)/CD38(-) for haematopoietic stem cells (HSCs), CD34(+)/ CD38(+)/CD45RA(-) for megakaryocyte-erythroid progenitors (MEPs), and CD34(+)/CD38(+)/CD45RA(+) for granulocytic-monocytic progenitors (GMPs) using regularised multinomial regression with three discrete outcomes and an elastic net penalty. The regularisation parameters were chosen by cross-validation, and MAGS assignment accuracy was validated in an independent data set (N = 38; accuracy = 0.79) of sorted normal myeloid subpopulations. The prognostic value of MAGS assignment was studied in two clinical cohorts (TCGA: N = 171; GSE6891: N = 520) and had a significant prognostic impact. Furthermore, multivariate Cox regression analysis using the MAGS subtype, FAB subtype, cytogenetics, molecular genetics, and age as explanatory variables showed independent prognostic value. Molecular characterisation of subtypes by differential gene expression analysis, gene set enrichment analysis, and mutation patterns indicated reduced proliferation and overrepresentation of RUNX1 and IDH2 mutations in the HSC subtype; increased proliferation and overrepresentation of CEBPA mutations in the MEP subtype; and innate immune activation and overrepresentation of WT1 mutations in the GMP subtype. We present a differentiationdependent classification system for AML subtypes with distinct pathogenetic and prognostic importance that can help identify candidates poorly responding to combination chemotherapy and potentially guide alternative treatments.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0229593