NCT07594925

Brief Summary

Microsatellite stable (MSS) locally advanced rectal cancer (LARC) remains a major therapeutic challenge despite advances in multimodal treatment. Colorectal cancer is the third most common malignancy worldwide and the second leading cause of cancer-related death. In China, rectal cancer accounts for nearly half of all colorectal cancers, with approximately 70% of patients presenting with locally advanced disease, which is associated with a high risk of recurrence and poor long-term survival. Neoadjuvant chemoradiotherapy followed by total mesorectal excision (TME) has become the standard treatment for LARC based on landmark trials such as CAO/ARO/AIO-94, NSABP-R03, and MRC-CR07, which demonstrated improved local control and reduced recurrence. However, the optimal neoadjuvant strategy remains under active investigation. Currently, long-course chemoradiotherapy and short-course radiotherapy (SCRT) are the two principal preoperative radiotherapy approaches. Long-course chemoradiotherapy achieves superior tumor downstaging and pathological complete response (pCR) rates but requires prolonged treatment duration and is associated with greater acute toxicity. In contrast, SCRT offers shorter treatment time, lower cost, and reduced toxicity. Importantly, delayed surgery after SCRT can significantly enhance tumor regression and achieve pCR rates comparable to those of long-course chemoradiotherapy. The development of total neoadjuvant therapy (TNT) has further transformed rectal cancer management by moving systemic chemotherapy to the preoperative setting, thereby improving treatment compliance, tumor response, and organ preservation. Among TNT strategies, consolidation chemotherapy after radiotherapy appears to provide superior tumor regression compared with induction chemotherapy. Immune checkpoint inhibitors targeting the PD-1/PD-L1 pathway have demonstrated remarkable efficacy in mismatch repair-deficient (dMMR)/microsatellite instability-high (MSI-H) rectal cancer. However, the majority of rectal cancers are mismatch repair-proficient/microsatellite stable (pMMR/MSS) tumors, which are generally considered immunologically "cold" and poorly responsive to immunotherapy alone. Radiotherapy can enhance antitumor immunity through increased antigen presentation, dendritic cell activation, CD8+ T-cell infiltration, and stimulation of systemic immune responses. Preclinical and clinical studies suggest synergistic effects between radiotherapy and immune checkpoint blockade. Several prospective studies combining chemoradiotherapy, chemotherapy, and immunotherapy in MSS LARC have reported encouraging pCR rates, particularly when immunotherapy is administered during the consolidation phase. SCRT-based TNT combined with immunotherapy has shown especially promising efficacy, with pCR rates exceeding those achieved with conventional chemoradiotherapy. Nevertheless, whether improved tumor regression can translate into durable survival benefits remains unclear. In this context, postoperative immunotherapy maintenance may represent an important strategy to further improve long-term disease control. Sintilimab is a fully human anti-PD-1 monoclonal antibody that restores T-cell-mediated antitumor immunity by blocking the PD-1/PD-L1 pathway. Previous studies have demonstrated favorable pharmacokinetics, durable receptor occupancy, and manageable toxicity profiles. Based on this rationale, we designed a prospective randomized phase II study to evaluate the efficacy and safety of SCRT sequentially combined with sintilimab and XELOX chemotherapy in MSS LARC. Patients in the experimental arm will receive SCRT followed by four cycles of XELOX plus sintilimab before TME surgery, followed by postoperative XELOX plus sintilimab and one year of immunotherapy maintenance. Patients in the control arm will receive SCRT combined with XELOX chemotherapy without maintenance immunotherapy. The primary endpoint is 3-year disease-free survival (3y-DFS). Secondary endpoints include pCR, objective response rate (ORR), overall survival (OS), 3-year OS rate, and treatment safety. This study aims to determine whether the addition of sintilimab and postoperative immunotherapy maintenance can improve long-term survival while maintaining acceptable safety. Through integration of radiotherapy, chemotherapy, and immunotherapy, this study seeks to establish a more effective TNT-based strategy for MSS rectal cancer.

Trial Health

77
On Track

Trial Health Score

Automated assessment based on enrollment pace, timeline, and geographic reach

Enrollment
130

participants targeted

Target at P75+ for phase_2

Timeline
46mo left

Started May 2026

Typical duration for phase_2

Geographic Reach
1 country

1 active site

Status
recruiting

Health score is calculated from publicly available data and should be used for screening purposes only.

Trial Relationships

Click on a node to explore related trials.

Study Timeline

Key milestones and dates

Study Progress2%
May 2026Mar 2030

Study Start

First participant enrolled

May 1, 2026

Completed
8 days until next milestone

First Submitted

Initial submission to the registry

May 9, 2026

Completed
10 days until next milestone

First Posted

Study publicly available on registry

May 19, 2026

Completed
3 years until next milestone

Primary Completion

Last participant's last visit for primary outcome

June 1, 2029

Expected
9 months until next milestone

Study Completion

Last participant's last visit for all outcomes

March 1, 2030

Last Updated

May 19, 2026

Status Verified

May 1, 2026

Enrollment Period

3.1 years

First QC Date

May 9, 2026

Last Update Submit

May 17, 2026

Conditions

Rectal Cancer

Keywords

rectal cancerImmunotherapyradiotherapychenmotherapy

Outcome Measures

Primary Outcomes (1)

  • DFS

    The time from the date of random assignment to the first occurrence of locoregional failure, DM, second primary tumor, or death from any cause.

    From date of randomization until the first documented disease progression, death from any cause, or last follow-up, whichever occurs first, assessed up to 36 months

Secondary Outcomes (2)

  • Overall survival

    From date of randomization until death from any cause or last follow-up, whichever occurs first, assessed up to 36 months

  • Toxicity

    From the first dose of study treatment until the last scheduled follow-up visit or study completion, whichever occurs first, assessed up to 36 months

Study Arms (2)

CRT plus immunotherapy group

EXPERIMENTAL

* Stage 1: Short-course radiotherapy combined with 4 cycles of XELOX regimen chemotherapy + sintilimab immunotherapy; * Stage 2: After surgery, receive 4 cycles of XELOX regimen chemotherapy + sintilimab immunotherapy, followed by immunotherapy maintenance until 1 year.

Drug: SintilimabDrug: Chemotherapy DrugsRadiation: radiotherapy

CRT group

ACTIVE COMPARATOR

* Stage 1: Short-course radiotherapy combined with 4 cycles of XELOX regimen chemotherapy; * Stage 2: After surgery, receive 4 cycles of XELOX regimen chemotherapy, followed by active surveillance.

Drug: Chemotherapy DrugsRadiation: radiotherapy

Interventions

SintilimabDRUG

* Stage 1: Short-course radiotherapy combined with 4 cycles of XELOX regimen chemotherapy + sintilimab immunotherapy; * Stage 2: After surgery, receive 4 cycles of XELOX regimen chemotherapy + sintilimab immunotherapy, followed by immunotherapy maintenance until 1 year. Sintilimab: 200mg, intravenous drip (ivgtt), day 1, once every 3 weeks, infused before chemotherapy drugs.

CRT plus immunotherapy group
Chemotherapy DrugsDRUG

* Capecitabine Administration: 1000 mg/m², twice daily, taken half an hour after meals, with a 12-hour interval between doses, administered continuously for 14 days (Days 1-14), repeated every 3 weeks (adjusted according to the degree of myelosuppression after chemotherapy in patients, adjustment within 75%-100% of the standard treatment dose intensity is allowed). * Oxaliplatin Administration: 130mg/m², day 1, repeated every 3 weeks. Oxaliplatin is dissolved in 500 mL of 5% glucose solution (to achieve a concentration above 0.2 mg/mL) and infused intravenously for 2-6 hours (adjusted according to the degree of myelosuppression after chemotherapy in patients, adjustment within 75%-100% of the standard treatment dose intensity is allowed).

CRT groupCRT plus immunotherapy group
radiotherapyRADIATION

* Irradiation Technology: Intensity-modulated radiation therapy (IMRT) is adopted. * Target Volume Definition and Delineation: * GTV Delineation: Primary tumor area, including the primary rectal lesion, corresponding regional mesorectum and metastatic lymph nodes; * CTV Delineation: Refer to Definition and delineation of the clinical target volume for rectal cancer. * PTV Delineation: On the basis of CTV, 0.5 cm is expanded in the left-right direction, and 1.0 cm is expanded in the anteroposterior and craniocaudal directions; * Normal tissues and organs to be delineated include: bilateral femoral heads, bladder, colon, small intestine within the irradiation range (to be delineated 3 layers above the PTV), and testes (in males). Irradiation Dose: Whole pelvic PTV: 25Gy/5 fractions/1 week Normal Tissue and Organ Dose Limits: Femoral head: V20 \< 5%; Bladder: V20 \< 50%; Colon: V20 \< 10%, Dmax \< 27Gy; Small intestine: V20 \< 10%, Dmax \< 26Gy.

CRT groupCRT plus immunotherapy group

Eligibility Criteria

Age18 Years - 75 Years
Sexall
Healthy VolunteersNo
Age GroupsAdult (18-64), Older Adult (65+)

You may qualify if:

  • Age 18-75 years, regardless of gender;
  • Stage II/III disease (cT3-T4N0 or cT2-4N+) without distant metastasis on magnetic resonance imaging (MRI) or endoscopic ultrasound (EUS), according to the 8th edition of the AJCC Cancer Staging Manual (2018);
  • The lower boundary of the lesion is ≤ 10 cm from the anal verge, confirmed by colonoscopy or digital rectal examination;
  • Pathologically confirmed or re-reviewed rectal adenocarcinoma;
  • Eastern Cooperative Oncology Group (ECOG) performance status of 0-1;
  • Meet the following laboratory diagnostic indicators:
  • Hemoglobin ≥ 90 g/L, white blood cell count ≥ 3.5×10⁹/L;
  • Neutrophil count ≥ 1.5×10⁹/L, platelet count ≥ 100×10⁹/L;
  • Creatinine ≤ 1.0×upper normal limit (UNL), blood urea nitrogen (BUN) ≤ 1.0×UNL;
  • Alanine aminotransferase (ALT) ≤ 1.5×UNL;
  • Aspartate aminotransferase (AST) ≤ 1.5×UNL;
  • Alkaline phosphatase (ALP) ≤ 1.5×UNL;
  • Total bilirubin (TBIL) ≤ 1.5×UNL;
  • Urinary protein (-); normal bleeding and coagulation time.
  • No history of allergy to platinum-based drugs;
  • +3 more criteria

You may not qualify if:

  • Previous treatment with anti-PD-1/L1, anti-CTLA-4 immunotherapeutic drugs, or other experimental immunotherapeutic agents;
  • Patients with severe autoimmune diseases: active inflammatory bowel disease (including Crohn's disease, ulcerative colitis), rheumatoid arthritis, scleroderma, systemic lupus erythematosus, autoimmune vasculitis (such as Wegener's granulomatosis), etc.;
  • Symptomatic interstitial lung disease or active infectious/non-infectious pneumonia;
  • Patients with risk factors for intestinal perforation: active diverticulitis, intra-abdominal abscess, gastrointestinal (GI) obstruction, abdominal cancer, or other known risk factors for intestinal perforation;
  • History of other malignant tumors, excluding curable non-melanoma skin cancer and carcinoma in situ of the cervix;
  • Patients with active infection, heart failure, myocardial infarction within 6 months, unstable angina pectoris, or unstable arrhythmia;
  • Physical examination or clinical laboratory findings that the investigator believes may interfere with the results or increase the risk of treatment complications in patients, or other uncontrollable diseases;
  • Lactating or pregnant women;
  • Congenital or acquired immunodeficiency diseases including human immunodeficiency virus (HIV), or history of organ transplantation or allogeneic stem cell transplantation;
  • Known active hepatitis B virus (HBV) infection (HBV-DNA ≥ 2000 U/mL), hepatitis C virus (HCV) infection, or active pulmonary tuberculosis infection;
  • Patients who have received tumor vaccines or other vaccines within 4 weeks before the start of treatment; (Note: Seasonal influenza vaccines for injection are mostly inactivated vaccines and thus allowed, while intranasal preparations are usually live attenuated vaccines and thus not allowed);
  • Patients receiving concurrent use of other immunomodulators, chemotherapeutic drugs, drugs in other clinical studies, or long-term cortisol therapy are not eligible for enrollment;
  • Patients with mental illness, substance abuse, or social problems that affect compliance will not be enrolled after review by doctors;
  • Patients with allergies or contraindications to the study drugs.

Contact the study team to confirm eligibility.

Sponsors & Collaborators

Study Sites (1)

Tianjin Medical University Cancer Institute & Hospital, Key Laboratory of Cancer Prevention and Therapy, National Clinical Research Center for Cancer, Tianjin's Clinical Research Center for Cancer

Tianjin, 300060, China

RECRUITING

MeSH Terms

Conditions

Rectal Neoplasms

Interventions

sintilimabAntineoplastic AgentsRadiotherapy

Condition Hierarchy (Ancestors)

Colorectal NeoplasmsIntestinal NeoplasmsGastrointestinal NeoplasmsDigestive System NeoplasmsNeoplasms by SiteNeoplasmsDigestive System DiseasesGastrointestinal DiseasesIntestinal DiseasesRectal Diseases

Intervention Hierarchy (Ancestors)

Therapeutic UsesPharmacologic ActionsChemical Actions and UsesTherapeutics

Central Study Contacts

Maobin Meng

CONTACT

+86 15202231270mmeng@tmu.edu.cn

Junfeng Wang

CONTACT

+86 18622228675

Study Design

Study Type
interventional
Phase
phase 2
Allocation
RANDOMIZED
Masking
NONE
Purpose
TREATMENT
Intervention Model
PARALLEL
Sponsor Type
OTHER
Responsible Party
SPONSOR

Study Record Dates

First Submitted

May 9, 2026

First Posted

May 19, 2026

Study Start

May 1, 2026

Primary Completion (Estimated)

June 1, 2029

Study Completion (Estimated)

March 1, 2030

Last Updated

May 19, 2026

Record last verified: 2026-05

Data Sharing

IPD Sharing
Will not share

Locations

CN(1)