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The creatine kinase pathway is a metabolic vulnerability in EVI1-positive acute myeloid leukemia

dc.contributor.authorBassil, Christopher F
dc.contributor.authorBen-Sahra, Issam
dc.contributor.authorBenajiba, Lina
dc.contributor.authorAlexe, Gabriela
dc.contributor.authorPikman, Yana
dc.contributor.authorConway, Amy S
dc.contributor.authorBurgess, Michael R
dc.contributor.authorLi, Qing
dc.contributor.authorLuciano, Frédéric
dc.contributor.authorAuberger, Patrick
dc.contributor.authorGalinsky, Ilene
dc.contributor.authorDeAngelo, Daniel J
dc.contributor.authorStone, Richard M
dc.contributor.authorZhang, Yi
dc.contributor.authorPerkins, Archibald S
dc.contributor.authorShannon, Kevin
dc.contributor.authorPuissant, Alexandre
dc.contributor.authorStegmaier, Kimberly
dc.contributor.authorFenouille, Nina
dc.contributor.authorRamos, Azucena
dc.contributor.authorHemann, Michael
dc.date.accessioned2018-06-26T15:01:12Z
dc.date.available2018-06-26T15:01:12Z
dc.date.issued2017-02
dc.identifier.issn1078-8956
dc.identifier.issn1546-170X
dc.identifier.urihttp://hdl.handle.net/1721.1/116620
dc.description.abstractExpression of the MECOM (also known as EVI1) proto-oncogene is deregulated by chromosomal translocations in some cases of acute myeloid leukemia (AML) and is associated with poor clinical outcome. Here, through transcriptomic and metabolomic profiling of hematopoietic cells, we reveal that EVI1 overexpression alters cellular metabolism. A screen using pooled short hairpin RNAs (shRNAs) identified the ATP-buffering, mitochondrial creatine kinase CKMT1 as necessary for survival of EVI1-expressing cells in subjects with EVI1-positive AML. EVI1 promotes CKMT1 expression by repressing the myeloid differentiation regulator RUNX1. Suppression of arginine-creatine metabolism by CKMT1-directed shRNAs or by the small molecule cyclocreatine selectively decreased the viability, promoted the cell cycle arrest and apoptosis of human EVI1-positive cell lines, and prolonged survival in both orthotopic xenograft models and mouse models of primary AML. CKMT1 inhibition altered mitochondrial respiration and ATP production, an effect that was abrogated by phosphocreatine-mediated reactivation of the arginine-creatine pathway. Targeting CKMT1 is thus a promising therapeutic strategy for this EVI1-driven AML subtype that is highly resistant to current treatment regimens. Keywords: AML; RUNX1; CKMT1; cyclocreatine; arginine metabolismen_US
dc.description.sponsorshipNational Cancer Institute (U.S.) (NIH 1R35 CA210030-01)en_US
dc.description.sponsorshipStand Up To Canceren_US
dc.description.sponsorshipBridge Projecten_US
dc.description.sponsorshipNational Cancer Institute (U.S.) (David H. Koch Institute for Integrative Cancer Research at MIT. Grant P30-CA14051)en_US
dc.publisherSpringer Natureen_US
dc.relation.isversionofhttp://dx.doi.org/10.1038/NM.4283en_US
dc.rightsArticle is made available in accordance with the publisher's policy and may be subject to US copyright law. Please refer to the publisher's site for terms of use.en_US
dc.sourcePMCen_US
dc.titleThe creatine kinase pathway is a metabolic vulnerability in EVI1-positive acute myeloid leukemiaen_US
dc.typeArticleen_US
dc.identifier.citationFenouille, Nina, et al. “The Creatine Kinase Pathway Is a Metabolic Vulnerability in EVI1-Positive Acute Myeloid Leukemia.” Nature Medicine, vol. 23, no. 3, Feb. 2017, pp. 301–13.en_US
dc.contributor.departmentMassachusetts Institute of Technology. Department of Biologyen_US
dc.contributor.departmentKoch Institute for Integrative Cancer Research at MITen_US
dc.contributor.mitauthorFenouille, Nina
dc.contributor.mitauthorRamos, Azucena
dc.contributor.mitauthorHemann, Michael
dc.relation.journalNature Medicineen_US
dc.eprint.versionAuthor's final manuscripten_US
dc.type.urihttp://purl.org/eprint/type/JournalArticleen_US
eprint.statushttp://purl.org/eprint/status/PeerRevieweden_US
dc.date.updated2018-06-21T17:15:18Z
dspace.orderedauthorsFenouille, Nina; Bassil, Christopher F; Ben-Sahra, Issam; Benajiba, Lina; Alexe, Gabriela; Ramos, Azucena; Pikman, Yana; Conway, Amy S; Burgess, Michael R; Li, Qing; Luciano, Frédéric; Auberger, Patrick; Galinsky, Ilene; DeAngelo, Daniel J; Stone, Richard M; Zhang, Yi; Perkins, Archibald S; Shannon, Kevin; Hemann, Michael T; Puissant, Alexandre; Stegmaier, Kimberlyen_US
dspace.embargo.termsNen_US
dc.identifier.orcidhttps://orcid.org/0000-0001-7168-8672
mit.licensePUBLISHER_POLICYen_US


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