Constitutive activation of RAS/MAPK pathway cooperates with trisomy 21 and is therapeutically exploitable in down syndrome b-cell leukemia

Anouchka P. Laurent, Aurelie Siret, Cathy Ignacimouttou, Kunjal Panchal, M'Boyba Diop, Silvia Jenni, Yi Chien Tsai, Damien Roos-Weil, Zakia Aid, Nais Prade, Stephanie Lagarde, Damien Plassard, Gaelle Pierron, Estelle Daudigeos, Yann Lecluse, Nathalie Droin, Beat C. Bornhauser, Laurence C. Cheung, John D. Crispino, Muriel GaudryOlivier A. Bernard, Elizabeth Macintyre, Carole Barin Bonnigal, Rishi S. Kotecha, Birgit Geoerger, Paola Ballerini, Jean Pierre Bourquin, Eric Delabesse, Thomas Mercher, Sebastien Malinge

    Résultats de recherche: Contribution à un journalArticleRevue par des pairs

    17 Citations (Scopus)

    Résumé

    Purpose: Children with Down syndrome (constitutive trisomy 21) that develop acute lymphoblastic leukemia (DS-ALL) have a 3-fold increased likelihood of treatment-related mortality coupled with a higher cumulative incidence of relapse, compared with other children with B-cell acute lymphoblastic leukemia (B-ALL). This highlights the lack of suitable treatment for Down syndrome children with B-ALL. Experimental Design: To facilitate the translation of new therapeutic agents into clinical trials, we built the first preclinical cohort of patient-derived xenograft (PDX) models of DS-ALL, comprehensively characterized at the genetic and transcriptomic levels, and have proven its suitability for preclinical studies by assessing the efficacy of drug combination between the MEK inhibitor trametinib and conventional chemotherapy agents. Results: Whole-exome and RNA-sequencing experiments revealed a high incidence of somatic alterations leading to RAS/MAPK pathway activation in our cohort of DS-ALL, as well as in other pediatric B-ALL presenting somatic gain of the chromosome 21 (B-ALLþ21). In murine and human B-cell precursors, activated KRASG12D functionally cooperates with trisomy 21 to deregulate transcriptional networks that promote increased proliferation and self renewal, as well as B-cell differentiation blockade. Moreover, we revealed that inhibition of RAS/MAPK pathway activation using the MEK1/2 inhibitor trametinib decreased leukemia burden in several PDX models of B-ALLþ21, and enhanced survival of DS-ALL PDX in combination with conventional chemotherapy agents such as vincristine. Conclusions: Altogether, using novel and suitable PDX models, this study indicates that RAS/MAPK pathway inhibition represents a promising strategy to improve the outcome of Down syndrome children with B-cell precursor leukemia.

    langue originaleAnglais
    Pages (de - à)3307-3318
    Nombre de pages12
    journalClinical Cancer Research
    Volume26
    Numéro de publication13
    Les DOIs
    étatPublié - 1 juil. 2020

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