Blood Cancer Journal (Jun 2023)

A Phase I study of Milademetan (DS3032b) in combination with low dose cytarabine with or without venetoclax in acute myeloid leukemia: Clinical safety, efficacy, and correlative analysis

  • Jayastu Senapati,
  • Muharrem Muftuoglu,
  • Jo Ishizawa,
  • Hussein A. Abbas,
  • Sanam Loghavi,
  • Gautam Borthakur,
  • Musa Yilmaz,
  • Ghayas C. Issa,
  • Samuel I. Dara,
  • Mahesh Basyal,
  • Li Li,
  • Kiran Naqvi,
  • Rasoul Pourebrahim,
  • Elias J. Jabbour,
  • Steven M. Kornblau,
  • Nicholas J. Short,
  • Naveen Pemmaraju,
  • Guillermo Garcia-Manero,
  • Farhad Ravandi,
  • Joseph Khoury,
  • Naval Daver,
  • Hagop M. Kantarjian,
  • Michael Andreeff,
  • Courtney D. DiNardo

DOI
https://doi.org/10.1038/s41408-023-00871-1
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 6

Abstract

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Abstract In TP53 wild-type acute myeloid leukemia (AML), inhibition of MDM2 can enhance p53 protein expression and potentiate leukemic cell apoptosis. MDM2 inhibitor (MDM2i) monotherapy in AML has shown modest responses in clinical trials but combining options of MDM2i with other potent AML-directed agents like cytarabine and venetoclax could improve its efficacy. We conducted a phase I clinical trial (NCT03634228) to study the safety and efficacy of milademetan (an MDM2i) with low-dose cytarabine (LDAC)±venetoclax in adult patients with relapsed refractory (R/R) or newly diagnosed (ND; unfit) TP53 wild-type AML and performed comprehensive CyTOF analyses to interrogate multiple signaling pathways, the p53-MDM2 axis and the interplay between pro/anti-apoptotic molecules to identify factors that determine response and resistance to therapy. Sixteen patients (14 R/R, 2 N/D treated secondary AML) at a median age of 70 years (range, 23–80 years) were treated in this trial. Two patients (13%) achieved an overall response (complete remission with incomplete hematological recovery). Median cycles on trial were 1 (range 1–7) and at a median follow-up of 11 months, no patients remained on active therapy. Gastrointestinal toxicity was significant and dose-limiting (50% of patients ≥ grade 3). Single-cell proteomic analysis of the leukemia compartment revealed therapy-induced proteomic alterations and potential mechanisms of adaptive response to the MDM2i combination. The response was associated with immune cell abundance and induced the proteomic profiles of leukemia cells to disrupt survival pathways and significantly reduced MCL1 and YTHDF2 to potentiate leukemic cell death. The combination of milademetan, LDAC±venetoclax led to only modest responses with recognizable gastrointestinal toxicity. Treatment-induced reduction of MCL1 and YTHDF2 in an immune-rich milieu correlate with treatment response.