| Literature DB >> 31300747 |
Richard Bisaillon1, Céline Moison1, Clarisse Thiollier1, Jana Krosl1, Marie-Eve Bordeleau1, Bernhard Lehnertz1, Vincent-Philippe Lavallée1,2, Tara MacRae1, Nadine Mayotte1, Caroline Labelle1,3, Geneviève Boucher1, Jean-François Spinella1, Isabel Boivin1, Giovanni D'Angelo4, Sylvie Lavallée4, Anne Marinier1,5, Sébastien Lemieux1,3, Josée Hébert1,2,4,6, Guy Sauvageau7,8,9,10.
Abstract
Acute myeloid leukemias (AML) with mutations in the NPM1 gene (NPM1c+) represent a large AML subgroup with varying response to conventional treatment, highlighting the need to develop targeted therapeutic strategies for this disease. We screened a library of clinical drugs on a cohort of primary human AML specimens and identified the BCL2 inhibitor ABT-199 as a selective agent against NPM1c+ AML. Mutational analysis of ABT-199-sensitive and -resistant specimens identified mutations in NPM1, RAD21, and IDH1/IDH2 as predictors of ABT-199 sensitivity. Comparative transcriptome analysis further uncovered BCL2A1 as a potential mediator of ABT-199 resistance in AML. In line with our observation that RAD21 mutation confers sensitivity to ABT-199, we provide functional evidence that reducing RAD21 levels can sensitize AML cells to BCL2 inhibition. Moreover, we demonstrate that ABT-199 is able to produce selective anti-AML activity in vivo toward AML with mutations associated with compound sensitivity in PDX models. Overall, this study delineates the contribution of several genetic events to the response to ABT-199 and provides a rationale for the development of targeted therapies for NPM1c+ AML.Entities:
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Year: 2019 PMID: 31300747 DOI: 10.1038/s41375-019-0485-x
Source DB: PubMed Journal: Leukemia ISSN: 0887-6924 Impact factor: 11.528