Involve-site Radiotherapy Combined With Chemotherapy and Immunotherapy as Neoadjuvant Treatment for Locally Advanced Rectal Cancer (REFIRT)

This study aims to provide stronger clinical evidence for involve-site short-course radiotherapy combined with immunotherapy as a neoadjuvant treatment strategy for locally advanced rectal cancer. The rationale for this trial is based on the limitations of standard radiotherapy, which uses large target volumes and results in significant toxicities, higher surgical complication rates, decreased patient compliance, reduced quality of life, and potentially compromised systemic therapy intensity. Reducing the radiation field is expected to lower treatment-related toxicity while preserving local tumor control and enhancing the efficacy of combined immunotherapy.

Study Objectives and Expected Outcomes The primary objective is to evaluate the safety and efficacy of involve-site short-course radiotherapy combined with chemotherapy and immunotherapy in patients with locally advanced rectal cancer, compared with conventional standard-field radiotherapy. The expected outcome is that the experimental regimen will demonstrate better safety, comparable or improved surgical resection and local control rates, and no higher incidence of distant metastasis relative to standard approaches.

Study Design and Methods This is a single-center, randomized, prospective, exploratory interventional trial. Due to the nature of the treatment, blinding is not feasible; thus, patients will be randomized in an open-label manner. Stratified randomization will be performed using block randomization with a block size of 6, and random sequences will be generated by the data management team.The study population will consist of 60 eligible patients who will be randomly assigned in equal numbers to three treatment groups (A, B, and C; 20 patients per group).

Group A (Control 1): Standard long-course radiotherapy (50 Gy in 25 fractions) combined with concurrent capecitabine chemotherapy, followed by four cycles of CAPOX chemotherapy and surgery, then four cycles of adjuvant CAPOX.

Group B (Control 2): Standard short-course radiotherapy (25 Gy in 5 fractions), followed two weeks later by four cycles of CAPOX chemotherapy plus sintilimab (anti-PD-1 immunotherapy), then surgery, followed by four cycles of adjuvant CAPOX.

Group C (Experimental): Involve-site short-course radiotherapy (25 Gy in 5 fractions), with the target volume limited to the primary tumor and involved lymph nodes as defined by MRI and CT imaging. One week after radiotherapy, patients will receive four cycles of CAPOX plus sintilimab, followed by surgery and then four cycles of adjuvant CAPOX.

Endpoints Primary Endpoint: Two-year local control rate (defined as the proportion of patients without pelvic recurrence or distant metastasis within 2 years after surgery).

Secondary Endpoints: Pathological complete response (pCR) rate, surgical resection rate, incidence of grade ≥3 radiation-induced proctitis, overall survival (OS), objective response rate (ORR), disease control rate (DCR), and incidence of severe postoperative complications (including anastomotic leakage, unplanned stoma, delayed wound healing beyond one month, severe infection, or thrombosis).

Patient Selection and Eligibility Eligible patients are those aged 18-75 years with histologically confirmed rectal adenocarcinoma, clinical stage T3-T4 and/or N+, and/or CRM-positive disease without lateral lymph node metastasis, and ECOG performance status of 0-1. Patients must not have received prior anticancer therapy and must provide signed informed consent.

Treatment and Follow-up Procedures Patients will undergo pre-treatment evaluation including physical examination, complete blood count, liver and renal function tests, tumor markers, electrocardiogram, pelvic MRI, and chest/abdominal contrast-enhanced CT. Follow-up evaluations will be performed every 3 months after surgery, and will continue until 24 months after the last patient undergoes surgery.

Data Collection and Outcome Assessment Tumor regression will be evaluated by MRI and pathological assessment according to Mandard tumor regression grading (TRG1-TRG5). Response will also be assessed by RECIST version 1.1 criteria.

Objective Response Rate (ORR): proportion of patients with CR or PR. Disease-Free Survival (DFS): time from surgery to recurrence, metastasis, or death.

Disease Control Rate (DCR): proportion of patients with CR, PR, or SD. Duration of Response (DOR): interval from initial response to progression or death.

Overall Survival (OS): time from randomization to death from any cause. Safety will be monitored and graded according to CTCAE version 5.0. The incidence, severity, and relationship of all adverse events (AEs), treatment-emergent AEs (TEAEs), serious AEs (SAEs), and immune-related AEs (irAEs) will be recorded. The number and proportion of patients requiring treatment modification or discontinuation due to AEs will be documented.

Statistical Analysis This exploratory trial will use a fixed sample size of 60 patients. Descriptive statistics will be used to summarize baseline characteristics. Continuous variables will be expressed as mean ± SD or median (range), while categorical variables will be summarized as frequency (percentage).

Study Timeline Planned enrollment period: 6 months. Planned follow-up: 24 months post-surgery. Total study duration: approximately 3 years. Study initiation: September 2025. Expected completion: August 2028.

Conclusion This trial is designed to evaluate whether involve-site short-course radiotherapy combined with chemotherapy and immunotherapy can achieve comparable local control while reducing toxicity and improving systemic outcomes in patients with locally advanced rectal cancer. The results are expected to provide new clinical evidence supporting optimized neoadjuvant strategies .