PRODIGE 90 - (FFCD 2204) Neoadjuvant Dostarlimab with Short Course Radiotherapy in a Watch-and-wait Strategy for Microsatellite Unstable or Mismatch Repair-deficient Locally Advanced Rectal Cancer Patients

Sponsor
Centre Hospitalier Universitaire Dijon
Study ID
NCT06762405
Phase
PHASE3
Status
Recruiting
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Conditions

  • Rectal Adenocarcinoma with Mismatch-repair Deficient (dMMR)/ Microsatellite Instability-high (MSI-H)

Eligibility Criteria

Sex
ALL
Age
18 Years - N/A
Healthy Volunteers
Not accepted

Interventions

  • radiotherapy — RADIATION
    short course of radiotherapy (5 grays × 5 days)
  • Dostarlimab — DRUG
    dostarlimab 500 mg intravenous infusion every 3 weeks for 6 months (nine cycles)
  • Biological study on circulating tumor DNA (optional for the patient) — BIOLOGICAL
    * Tissue collection (3 time points: baseline, w12 and 25) for: * Exome (on tumor and normal tissue), * 3'RNAseq, * Hiplex Immunofluorescence * In addition, 48 patients will be tested for Spatial transcriptomics assuming that 24 patients may have non-complete response and/or local recurrence and/or metastatic recurrence and will be paired with 24 patients with complete response and free of any disease at 2 years. * Blood collection (5 time points: baseline, w3, 6, 12 and 24) for: * ctDNA * Cytokine dosage * Proteomic analyses * Stool collection (3 time points: baseline, w3 and 24) for: Microbiota analyses

Study Details

Total neoadjuvant treatment (TNT) including radiotherapy and induction or consolidation systemic chemotherapy has become the standard treatment for patients with stage II and III rectal adenocarcinoma. Along with the improvement of DFS, this preoperative treatment has paved the way to a paradigm-shifting nonoperative management. Indeed, rectal preservation has become a new goal for patients without detectable residual cancer after TNT with the option to reserve surgery for those with cancer regrowth (25-40%). Five to 10% of non-metastatic rectal cancer patients are molecularly characterized as microsatellite unstable (MSI) or mismatch repair-deficient (dMMR), and present a decreased response to systemic chemotherapy. As this tumor phenotype is associated with high immunogenicity, immunotherapy with anti-PD1 molecules has recently emerged as the new standard first line treatment in the metastatic setting, with long duration of cancer control for at least 40% of patients. In patients with localized rectal tumors, it has been suggested that immunotherapy alone may induce complete clinical response and may allow these patients to be considered for nonoperative therapeutic approaches. Finally, given the efficacy of immunotherapy in MSI rectal patients, we did not want to differ for 5 weeks this treatment with the risk of disease progression by given long-course RT. In the present trial, radiotherapy is evaluated as a " potentiating " treatment for immunotherapy rather than as a " local treatment " in a TNT strategy.

Key Dates

Start date
Feb 6, 2025
Status verified
Feb 2025
Primary completion
Sep 30, 2030
Completion
Sep 30, 2030

Study Design

Enrollment
68 participants (estimated)
Allocation
RANDOMIZED
Intervention model
PARALLEL
Primary purpose
TREATMENT

Arms

  • Experimental: Radiotherapy followed by Dostarlimab arm
  • Active Comparator: Dostarlimab alone arm

Primary Outcome Measure

Treatment strategy failure (TSF) rate. [ Time Frame: at 24 months ]

Central Contacts