Single Versus Double Induction with "7+3" Containing 60 Versus 90 Mg Daunorubicin for Newly Diagnosed AML: Results from the Randomized Controlled SAL Dauno-Double Trial
Christoph Röllig, Björn Steffen, Christoph Schliemann, Jan‐Henrik Mikesch, Nael Alakel, Regina Herbst, Mathias Haenel, Richard Noppeney, Maher Hanoun, Martin Kaufmann, Zdeněk Ráčil, Kerstin Schäfer‐Eckart, Tim Sauer, Andreas Neubauer, Claudia D. Baldus, Jolana Mertová, Edgar Jost, Dirk Niemann, Jan Novák, Stefan W. Krause, Sebastian Scholl, Andreas Hochhaus, Gerhard Held, Tomáš Szotkowski, Christoph Schmid, Andreas Rank, Lars Fransecky, Michael Krämer, Frank Fiebig, Annett Haake, Friedrich Stoelzel, Johannes Schetelig, Jan Moritz Middeke, Uwe Platzbecker, Christian Thiede, Carsten Müller‐Tidow, Wolfgang E. Berdel, Hubert Serve, Gerhard Ehninger, Jiří Mayer, Martin Bornhaeuser
Abstract
Background A combination of cytarabine plus anthracycline according to the 7+3 schedule is the standard treatment backbone of fit newly diagnosed AML patients (pts). A daunorubicin dose of 90 mg/m2 is superior to 45 mg/m2, whereas little difference seems to be between 60 mg/m2 and 90 mg/m2. Double induction is commonly performed in younger pts in order to maximize dose intensity upfront. However, for pts with a good early response after first induction, there is no prospective randomized evidence on the necessity or value of a second induction cycle (IC). Aims To provide randomized evidence for two fundamental questions in standard induction: First, is 60 mg/m2 really sufficient for induction or is 90 mg/m2 more efficacious? Second, can good responders after the first 7+3 induction be spared a second IC? Methods DaunoDouble was a two-part, two-arm open-label multicenter prospective randomized phase III trial. Pts 18-65 years with newly diagnosed AML, normal cardiac and organ function received a first IC with seven days of cytarabine plus three days of daunorubicin ("7+3") with a 1:1 stratified randomization for 60 versus (vs) 90 mg/m2 (Dauno60 vs Dauno90). Response assessment in bone marrow was evaluated by cytology on day 15. A blast count <5% was defined as good response, which was the primary endpoint of this first randomization step. Good responders were randomized to receive a second IC (arm D) or no second IC (arm S). In arm D, the second IC contained 60 mg/m2 after Dauno60 and 45 mg/m2 after Dauno90. Primary endpoint of the second randomization was CR/CRi after completion of induction. We assumed non-inferiority of single induction in terms of CR/CRi rate, based on a margin of 7.5%. Results Between 2014 and 2022, 864 pts were enrolled and received the first IC with 7+3. Median age was 52 years, 88% had de novo AML. Favorable, intermediate and adverse risk (ELN 2017) was present in 37%, 46% and 17% of pts, respectively. No significant imbalances were observed between the two treatment arms except for a higher NPM1 mutant rate in the Dauno90 arm (32.4% vs 41.7%, p=0.034). A pre-planned interim analysis after the first randomization of 218 pts revealed a statistically and clinically non-significant difference of 42% vs 49% good responders after first induction with 60 vs 90 mg/m2 daunorubicin (p=0.341). Based on this result, the first randomization step was suspended and all consecutive pts received 60 mg/m2 in induction I. At the end of enrollment, 707 and 157 pts have received 60 or 90 mg/m2, with a corresponding proportion of good early responders of 44.4% vs 47.8% (p=0.930) and a CR rate of 89.6% vs 88.5% after the end of induction (p=0.691). After a median follow-up of 43.6 months, 3-y RFS after Dauno60 vs Dauno90 was 53.8% vs 50.1% (p=0.561) and 3-y OS 65.2% vs 58.3% (p=0.196). During first induction, 57% of pts in Dauno60 and 58% in Dauno90 experienced an AE ≥ grade 3 (p=0.877); mortality in induction I was 2.3% and 4.7%, respectively (p=0.109). After IC I, a marrow blast clearance below 5% on day 15 was achieved in 389 pts (45%), providing eligibility for the second randomization. Of these pts, 189 were randomized into arm S and 187 into arm D (ITT population). CR/CRi rates at the end of induction were 85.2% after single induction and 85.6% after double induction, resulting in a CR difference of 0.4% (p for non-inferiority test 0.0269). The CR/CRi rates in 326 pre-defined per-protocol pts (PP) were 86.8% vs 91.5%, resulting in a CR difference of 4.7% (p=0.205). Until the end of induction, 58% of pts in the S arm and 65% of pts in the D arm experienced an AE ≥ grade 3 (p=0.195). Early mortality 60 days after induction start was 0.6% in both arms. After a median follow-up time of 43.6 months, 3-y RFS after single vs double induction was 51% vs 60%, which was non-significant in the ITT population (HR 1.35; p=0.074) and borderline significant in the PP population (HR 1.43; 0=0.05), but not significant in multivariable analyses. OS after 3 years was identical with 77% vs 75% after single or double induction in the ITT (HR 1.02; p= 0.914) and 77% vs 76% in the PP population (HR 1.12; p=0.628). Conclusion The use of 90 mg daunorubicin in the context of classical 7+3 induction did not lead to higher remission rates or longer survival than 60 mg. In pts with a good early response after first induction, a second induction had only limited impact on RFS. Double induction did not lead to an overall survival benefit in pts with a good early response first 7+3 induction. Figure 1View largeDownload PPTFigure 1View largeDownload PPT Close modal