A multicenter, randomized study of decitabine as epigenetic priming with induction chemotherapy in children with AML

Lia Gore; Timothy J. Triche; Jason E. Farrar; Daniel Wai; Christophe Legendre; Gerald C. Gooden; Winnie S. Liang; John Carpten; David Lee; Frank Alvaro; Margaret E. Macy; Carola Arndt; Philip Barnette; Todd Cooper; Laura Martin; Aru Narendran; Jessica Pollard; Soheil Meshinchi; Jessica Boklan; Robert J. Arceci; Bodour Salhia

doi:10.1186/s13148-017-0411-x

Clinical Epigenetics (Oct 2017)

A multicenter, randomized study of decitabine as epigenetic priming with induction chemotherapy in children with AML

Lia Gore,
Timothy J. Triche,
Jason E. Farrar,
Daniel Wai,
Christophe Legendre,
Gerald C. Gooden,
Winnie S. Liang,
John Carpten,
David Lee,
Frank Alvaro,
Margaret E. Macy,
Carola Arndt,
Philip Barnette,
Todd Cooper,
Laura Martin,
Aru Narendran,
Jessica Pollard,
Soheil Meshinchi,
Jessica Boklan,
Robert J. Arceci,
Bodour Salhia

Affiliations

Lia Gore: Children’s Hospital Colorado and University of Colorado School of Medicine
Timothy J. Triche: Department of Translational Genomics and Norris Comprehensive Cancer Center, Jane Anne Nohl Division of Hematology, Keck School Medicine of University of Southern California
Jason E. Farrar: Arkansas Children’s Research Institute and University of Arkansas for Medical Sciences
Daniel Wai: Ron Matricaria Institute of Molecular Medicine
Christophe Legendre: Translational Genomics Research Institute
Gerald C. Gooden: Department of Translational Genomics and Norris Comprehensive Cancer Center, Jane Anne Nohl Division of Hematology, Keck School Medicine of University of Southern California
Winnie S. Liang: Translational Genomics Research Institute
John Carpten: Translational Genomics Research Institute
David Lee: Sidney Kimmel Comprehensive Cancer Center at Johns Hopkins’ University
Frank Alvaro: John Hunter Hospital
Margaret E. Macy: Children’s Hospital Colorado and University of Colorado School of Medicine
Carola Arndt: Mayo Clinic
Philip Barnette: Primary Children’s Medical Center and the University of Utah
Todd Cooper: Children’s Healthcare of Atlanta
Laura Martin: Nationwide Children’s Hospital
Aru Narendran: Alberta Children’s Hospital and University of Calgary
Jessica Pollard: Seattle Children’s Hospital
Soheil Meshinchi: Fred Hutchinson Cancer Research Center
Jessica Boklan: Phoenix Children’s Hospital
Robert J. Arceci: Ron Matricaria Institute of Molecular Medicine
Bodour Salhia: Department of Translational Genomics and Norris Comprehensive Cancer Center, Jane Anne Nohl Division of Hematology, Keck School Medicine of University of Southern California

DOI: https://doi.org/10.1186/s13148-017-0411-x
Journal volume & issue: Vol. 9, no. 1
pp. 1 – 13

Abstract

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Abstract Background Decitabine is a deoxycytidine nucleoside derivative inhibitor of DNA-methyltransferases, which has been studied extensively and is approved for myelodysplastic syndrome in adults but with less focus in children. Accordingly, we conducted a phase 1 multicenter, randomized, open-label study to evaluate decitabine pre-treatment before standard induction therapy in children with newly diagnosed AML to assess safety and tolerability and explore a number of biologic endpoints. Results Twenty-four patients were fully assessable for all study objectives per protocol (10 in Arm A = epigenetic priming induction, 14 in Arm B = standard induction). All patients experienced neutropenia and thrombocytopenia. The most common grade 3 and 4 non-hematologic adverse events observed were gastrointestinal toxicities and hypophosphatemia. Plasma decitabine PK were similar to previously reported adult data. Overall CR/CRi was similar for the two arms. MRD negativity at end-induction was 85% in Arm A versus 67% in Arm B patients. DNA methylation measured in peripheral blood over the course of treatment tracked with blast clearance and matched marrow aspirates at day 0 and day 21. Unlike end-induction marrow analyses, promoter methylation in blood identified an apparent reversal of response in the lone treatment failure, 1 week prior to the patient’s marrow aspirate confirming non-response. Decitabine-induced effects on end-induction (day 35–43 following initiation of treatment) marrows in Arm A were reflected by changes in DNA methylation in matched paired marrow diagnostic aspirates. Conclusions This first-in-pediatrics trial demonstrates that decitabine prior to standard combination chemotherapy is feasible and well tolerated in children with newly diagnosed AML. Pre-treatment with decitabine may represent a newer therapeutic option for pediatric AML, especially as it appears to induce important epigenetic alterations. The novel biological correlates studied in this trial offer a clinically relevant window into disease progression and remission. Additional studies are needed to definitively assess whether decitabine can enhance durability responses in children with AML. Trial registration NCT01177540

Published in Clinical Epigenetics

ISSN: 1868-7083 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General): Genetics
Website: https://clinicalepigeneticsjournal.biomedcentral.com/

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