634 Background: EV + pembro is the preferred standard 1L therapy for patients with locally advanced or metastatic UC (la/mUC). The randomized, open-label phase 1/2 substudy 04B in the KEYMAKER-U04 umbrella study (NCT05845814) aimed to build on the efficacy of this combination and evaluated EV + pembro–containing ICI coformulations and EV + pembro as 1L treatment in participants (pts) with la/mUC. Methods: Adult pts without prior systemic therapy for la/mUC and an ECOG PS of 0-1 were randomized 1:1:1 to EV + coformulated favezelimab (fave; anti–LAG3)/pembro 800 mg/200 mg (arm A), EV + coformulated vibostolimab (vibo; anti-TIGIT)/pembro 200 mg/200 mg (arm B), and EV + pembro 200 mg (arm C). Pts received EV 1.25 mg/kg IV on d1 and d8 Q3W until disease progression, intolerable toxicity, or study withdrawal, and pembro or pembro-containing coformulations IV on d1 Q3W for ≤2 years. A safety lead-in was performed for the first 10 pts in each of EV + fave/pembro and EV + vibo/pembro arms per modified toxicity probability interval with dose-limiting toxicity (DLT) monitoring in cycle 1. Primary end points: ORR per RECIST v1.1 by blinded independent central review (BICR) and safety. Secondary end points: PFS and DOR per RECIST v1.1 by BICR. Results: 124 pts received treatment (arm A: n = 41; arm B: n = 41; arm C: n = 42). Median follow-up (time from randomization to data cutoff Dec 16, 2024) (range) was 11.9 mo (9.7-17.0), 11.7 mo (9.7-16.3), and 11.8 mo (9.8-16.8), respectively. Most pts were male (74%); median age was 69 yrs. DLT was reported for 1/10 pts on EV + fave/pembro and no pts on EV + vibo/pembro. Efficacy results are in the table. Any-grade TRAEs were similar across all arms (arm A: 100%; arm B: 100%; arm C: 97.6%); grade ≥3 TRAEs were reported for 56.1%, 73.2%, and 61.9% of pts, respectively. Immune-mediated AEs and infusion reactions were reported for 65.9% pts in arm A, 53.7% in arm B, and 42.9% in arm C; immune-mediated AEs with > 10% higher incidence in any EV + pembro-containing ICI coformulation were hypothyroidism (31.7%, 14.6%, and 2.4%, respectively), severe skin reactions (24.4%, 29.3%, and 14.3%, respectively), hyperthyroidism (22.0%, 4.9%, and 4.8%, respectively), and infusion reactions (17.1%, 2.4%, and 0%, respectively). Conclusions: In pts with la/mUC, the addition of LAG3- or TIGIT-targeted ICIs to EV + pembro did not have a clinically significant impact on efficacy. No new safety signals were identified. Incidence of certain immune-mediated AEs was higher with pembro-containing coformulations compared to EV + pembro. Clinical trial information: NCT05845814 . Arm An = 41 Arm Bn = 41 Arm Cn = 42 ORR, % (95% CI) 66 (49-80) 59 (42-74) 57 (41-72) CR, n (%) 5 (12) 9 (22) 3 (7) DOR, median mo (range) NR (4.1 to 14.7+) 12.3 (2.5+ to 12.3) 12.1 (2.0+ to 12.1) PFS, median mo (95% CI) 11.3 (8.2-NR) 14.1 (5.1-NR) 10.9 (6.4-NR) 12-mo PFS rate, % (95% CI) 40.1 (15.1-64.3) 54.2 (37.4-68.3) 36.2 (18.9-53.9)
Heijden et al. (Sun,) studied this question.