Precision medicine treatment in acute myeloid leukemia using prospective genomic profiling: feasibility and preliminary efficacy of the Beat AML Master Trial.
Amy BurdRoss L LevineAmy S RuppertAlice S MimsUma BorateEytan M SteinPrapti PatelMaria R BaerWendy StockMichael W DeiningerWilliam BlumGary SchillerRebecca OlinMark LitzowJames ForanTara L LinBrian BallMichael BoyiadzisElie TraerOlatoyosi OdenikeMartha ArellanoAlison WalkerVu H DuongTibor KovacsovicsRobert H CollinsAbigail B ShobenNyla A HeeremaMatthew C FosterJo-Anne VergilioTim BrennanChristine VietzEric SeversonMolly MillerLeonard RosenbergSonja MarcusAshley YocumTimothy ChenMona StefanosBrian J DrukerJohn C ByrdPublished in: Nature medicine (2020)
Acute myeloid leukemia (AML) is the most common diagnosed leukemia. In older adults, AML confers an adverse outcome1,2. AML originates from a dominant mutation, then acquires collaborative transformative mutations leading to myeloid transformation and clinical/biological heterogeneity. Currently, AML treatment is initiated rapidly, precluding the ability to consider the mutational profile of a patient's leukemia for treatment decisions. Untreated patients with AML ≥ 60 years were prospectively enrolled on the ongoing Beat AML trial (ClinicalTrials.gov NCT03013998 ), which aims to provide cytogenetic and mutational data within 7 days (d) from sample receipt and before treatment selection, followed by treatment assignment to a sub-study based on the dominant clone. A total of 487 patients with suspected AML were enrolled; 395 were eligible. Median age was 72 years (range 60-92 years; 38% ≥75 years); 374 patients (94.7%) had genetic and cytogenetic analysis completed within 7 d and were centrally assigned to a Beat AML sub-study; 224 (56.7%) were enrolled on a Beat AML sub-study. The remaining 171 patients elected standard of care (SOC) (103), investigational therapy (28) or palliative care (40); 9 died before treatment assignment. Demographic, laboratory and molecular characteristics were not significantly different between patients on the Beat AML sub-studies and those receiving SOC (induction with cytarabine + daunorubicin (7 + 3 or equivalent) or hypomethylation agent). Thirty-day mortality was less frequent and overall survival was significantly longer for patients enrolled on the Beat AML sub-studies versus those who elected SOC. A precision medicine therapy strategy in AML is feasible within 7 d, allowing patients and physicians to rapidly incorporate genomic data into treatment decisions without increasing early death or adversely impacting overall survival.
Keyphrases
- acute myeloid leukemia
- end stage renal disease
- allogeneic hematopoietic stem cell transplantation
- palliative care
- chronic kidney disease
- newly diagnosed
- ejection fraction
- type diabetes
- randomized controlled trial
- healthcare
- stem cells
- combination therapy
- mesenchymal stem cells
- acute lymphoblastic leukemia
- bone marrow
- high dose
- patient reported outcomes
- low dose
- machine learning
- phase ii
- study protocol
- copy number
- advanced cancer
- placebo controlled
- single molecule
- drug induced