DREAMseq: A phase III trial of treatment sequences in BRAFV600-mutant (m) metastatic melanoma (MM)—Final clinical results.
M.B. Atkins, Sandra J. Lee, Bartosz Chmielowski, Ahmad A. Tarhini, Gary I. Cohen, Geoffrey T. Gibney, Thach‐Giao Truong, Diwakar Davar, Joe Stephenson, Brendan D. Curti, Joanna M. Brell, Kari Kendra, Alexandra P. Ikeguchi, Zihe Song, Samantha Guild, Jedd D. Wolchok, Antoni Ribas, John M. Kirkwood
Abstract
9506 Background: The DREAMseq trial compared efficacy and toxicity of the sequence of nivolumab/ipilimumab (N/I) followed by dabrafenib/trametinib (D/T) to the reverse sequence in patients (pts) with BRAFV600m MM. In 9/2021, with 59% of pts 2+ years (yr) from enrollment, the DSMC and NCI CTEP recommended halting the trial and releasing data that showed a 20% difference in 2-yr OS (72% vs 52%) favoring the N/I first sequence. Here we update data to median ~5 yr from entry and report secondary analyses including time to CNS relapse and percent unconfirmed responses (ucOR). Methods: Eligible pts with untreated BRAFV600m MM were stratified by ECOG Performance Status 0 or 1 and LDH, and randomized 1:1 to Step 1 treatment with either N/I (Arm A) or D/T (Arm B) and at disease progression (PD) were eligible for Step 2 alternate therapy, D/T (Arm C) or N/I (Arm D). Imaging was done at baseline and q12 weeks (wks). The primary endpoint was 2-yr OS. Secondary endpoints included: 3-yr OS, efficacy (PFS, ORR and DOR) and toxicity. Results: 267 out of 300 proposed pts were enrolled (135 Arm A; 132 Arm B). As of 7/23/24, median follow-up of 58 months (mo) (range:0-101), 30 pts had switched to Arm C and 52 to Arm D. 2-yr OS for those assigned to Arm A was 68.3% (95% CI: 60.8-76.9) and for Arm B 54.1% (95% CI: 46.1-63.7%) (log-rank p < 0.01). 3 and 5-yr OS by sequence and 2, 3 and 5-yr PFS for initial arms, and median PFS, ORR and DOR for all arms are shown in Table. There were 125 deaths (Arm A-C:47; Arm B-D:78). 76% of responders in Arm A and 24% in Arm B remain in response. At 12 wks, 59 pts on Arm A and 85 on Arm B had RECIST PR of which 10 (16.9%) and 35 (41.2%), respectively were ucOR by wk 24. CNS was the first site of PD in 24 pts on Arm A and 44 pts on Arm B. Median time to CNS PD: Arm A 12.2 mo (0.7-46.5); Arm B 8.4 mo (1.3-78.1) (p < 0.01). Conclusions: At nearly 5 yr median f/up, the N/I first treatment sequence continues to show superior efficacy over the D/T first sequence for treatment-naïve BRAFV600m MM with a near doubling (30% absolute difference) in 5-yr OS and a tripling of 5-yr PFS. While confirmed ORR were similar between Arms A and B, shorter DOR and more ucOR and more and earlier CNS PD were seen with initial D/T contributing to its worse efficacy. Clinical trial information: NCT02224781 . Secondary Endpoint (95% CI) Arm A to C (n=135) Arm B to D (n=132) Log-rank p 3 yr OS rate 65.6% (57.3, 73.9) 44.8% (36.7, 54.6) p<0.01 5 yr OS rate 63.3% (55.4, 72.3) 33.9% (25.9, 44.3) 2 yr PFS rate Arm A50.8% (42.8, 60.3) Arm B22.9% (16.5, 31.7) p<0.01 3 yr PFS rate 45.0% (37.0, 54.8) 15.9% (10.5, 24.0) 5 yr PFS rate 39.4% (31.3, 49.5) 12.8% (7.9, 20.7) Median PFS (mo) Arm A26.7 (11.2-47.3) Arm B8.5 (8.1-12.6) Arm C (n=30)11.2 (9.5, 22.3) Arm D (n=52)5.9 (2.9, 22.4) ORR Arm A (n= 132)51.5% (42.7, 60.3) Arm B (n=131)51.1% (42.3, 60.0) Arm C (n=30)70% (37.4, 74.5) Arm D (n= 52)46.2% (32.2, 60.5) Median DOR (mo) Arm A (n=68)Not reached Arm B (n=67)15.5 (11.2, 23.5) <0.01 Arm C (n=17)14.7 (8.2, NR) Arm D (n=20)45.2 (19.5, NR) p=0.03