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First results of SURE-02: A phase 2 study of neoadjuvant sacituzumab govitecan (SG) plus pembrolizumab (Pembro), followed by response-adapted bladder sparing and adjuvant pembro, in patients with muscle-invasive bladder cancer (MIBC).

Andrea Necchi, Joep de Jong, J. Proudfoot, Brigida Anna Maiorano, Antonio Cigliola, Valentina Tateo, Chiara Mercinelli, Michela Ravasi, Elai Davicioni, Marco Moschini, Giorgio Brembilla, Maurizio Colecchia, Francesco De Cobelli, Alberto Briganti, Francesco Montorsi

2025Journal of Clinical Oncology10 citationsDOI

Abstract

4518 Background: Standard of care for MIBC is radical cystectomy (RC) with neoadjuvant chemotherapy (CT), but ~50% of patients (pts) are ineligible for/refuse CT and survival for RC alone is dismal. Neoadjuvant Pembro and SG monotherapies showed activity in MIBC within PURE-01 and SURE-01 studies. SURE-02 (NCT05535218) is a phase 2 study of neoadjuvant SG+Pembro and adjuvant Pembro, including a bladder-sparing approach depending on clinical response. We report results of a prespecified interim analysis. Methods: Pts age ≥18 y, ECOG PS 0-1, with histologically confirmed cT2-T4N0M0 MIBC, ineligible/refusing CT, and scheduled for RC received 4 cycles of Pembro 200 mg on D1 and SG 7.5 mg/Kg on D1 and D8, Q3W, followed by postsurgical Pembro x 13 cycles, Q3W. A reTURBT is allowed instead of RC, followed by Pembro x 13 cycles, for pts achieving a clinical complete response (cCR), stringently defined as a negative magnetic resonance imaging (MRI) and no residual viable tumor at reTURBT (ypT0). Primary outcome measure is cCR rate: H0≤30%, H1≥45%. Other outcomes: ypT≤1N0-x rate including pts undergoing RC, safety (CTCAE v.5.0), survival. The total sample size is 48 pts in a 2-stage design, with 23 pts enrolled at first stage (≥7 cCR needed). Decipher Bladder (Veracyte, San Diego, CA) was used for transcriptome-wide analyses of primary TURBT tissue. Results: From 10/23 to 01/25, 40 pts were treated and 31 were efficacy evaluable. 20 (64.5%) had a cT2 stage, 12 (38.7%) had a centrally confirmed variant histology. The cCR-rate was 38.7% (N = 12; 95%CI: 21.8-57.8); all these pts underwent a reTURBT; ypT≤1N0-x rate was 51.6% (N = 16). Grade ≥3 treatment-related adverse-events occurred in 4 pts (12.9%), 2 dose omissions of SG and one dose delay (1W) were recorded. No SG dose-reduction was needed. cCR varied by molecular subtype. Transcriptome results were available for 23 pts: complete pathologic (ypT0) responses varied by Genomic Subtyping Classifier (GSC) groups with luminal tumors showing higher ypT0 rates vs non-luminal (73 vs 25%, p = 0.04). Similarly, based on Lund subtypes, genomically unstable (GU) tumors had ypT0 response in 67%, vs 57% for urothelial-like, 20% for basal/squamous and 0% for neuroendocrine-like. Higher stromal signature (> median) was associated with non-ypT0 response (p = 0.004), while neither Trop2 (p = 0.15) nor TOP1 (p = 0.79) gene expression were associated with ypT0 response. Conclusions: Perioperative SG+Pembro revealed a compelling cCR rate, with a manageable safety profile, allowing a bladder preservation in ~40% of pts. Pre-treatment molecular biomarker analyses suggest a unique tumor profile associated with cCR. Overall, SURE-02 interim results support the completion of study accrual and further investigation of SG+Pembro in pts with MIBC. Clinical trial information: NCT05535218 .

Topics & Concepts

MedicinePembrolizumabBladder cancerAdjuvantUrologySurgeryOncologyInternal medicineCancerImmunotherapyBladder and Urothelial Cancer TreatmentsCancer Immunotherapy and BiomarkersUrinary and Genital Oncology Studies