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

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

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