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Though surgical resection remains the primary choice for advanced rectal cancer, about 80% are considered unresectable due to the number, size, or location of metastases. The overall prognosis of patients who accepted traditional treatment methods is still poor. Therefore, the investigators designed a combination therapy, short-course radiotherapy followed by chemotherapy with target therapy and anti-PD-1 immunotherapy. This study implement the combination therapy in patients with rectal cancer who are initially unresectable in the locally advanced stage with multiple liver/pulmonary metastases, to evaluate whether they can improve the objective response rate, the conversion rate of radical surgery and prolong the overall survival of patients, and strive to provide high-level medical evidence for the clinical treatment.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| unresectable group | Experimental | Patients will receive tislelizumab in combination with radiotherapy and targeted therapy. 2 weeks after large fractionated radiotherapy for primary rectum lesion and metastasis, patients will be treated with systemic treatment including chemotherapy combined with targeted therapy and immunotherapy. Patients will be evaluated by MDT every 2 months since the beginning of the treatment. Those who are regarded as NED will be treated surgically/locally. Those in stable or partial remission will continue with combination therapy. Those with progressive disease will be withdrawn from study. Patients who are not surgically treatable will continue with combination therapy until disease progression or receiving surgical treatment. |
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| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| a combination therapy including tislelizumab | Combination Product | For liver/pulmonary metastasis, the treatment plan is to implement large fraction radiotherapy for 4-8 times. For primary rectum lesion, short-course radiotherapy regimen through intensity-modulated radiotherapy will be applied with dose of 25Gy/5Fx. Immunotherapy contains anti-PD-1 monoclonal antibody, Tislelizumab(200mg, d1, q3w, i.v). For patients with RAS or BRAF mutation, chemotherapy adopts FOLFOX+BEV plan. For patients without RAS or BRAF mutation, chemotherapy adopts FOLFIRI+CET plan. Patients will be followed for safety during the study. The safety follow-up period is defined as 90 days after the last dose of tislelizumab. Safety related data will be collected from the time of signing the informed consent until the end of the safety follow-up period or the start of new therapy. |
| Measure | Description | Time Frame |
|---|---|---|
| Early Tumor Shrinkage | The relative change of the sum of the longest diameters of the baseline RECIST target lesion at 8 weeks of systemic therapy, distinguished by 20% as the cut-off point between early response and no response. | 5 years after intervention |
| Measure | Description | Time Frame |
|---|---|---|
| Disease Control Rate | Percentage of patients with disease control in non-irradiated metastatic lesions | 5 years after intervention |
| Duration of Response | The time between PR/CR and subsequent progressive disease or death of any cause. |
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Inclusion Criteria:
Age 18~70;
Patient signs informed consent;
ECOG score 0~1;
Initial colonoscopy and pathology: adenocarcinoma;
MRI: rectal cancer located less than 10cm from the anus;
Imaging confirms multiple measurable metastases exist in the liver or lung , which are evaluated as NED unacceptable by MDT discussion;
no previous treatment;
Patients have adequate organ function;
No contraindications to surgery or chemoradiation;
The relevant test results within 7 days before the first dose must meet the following requirements:
Blood routine examination (no blood transfusion within 7 days before screening, no correction with hematopoietic stimulating factor drugs):
Blood chemistry (no blood transfusion or albumin within 7 days prior to screening):
TSH is within the normal range; if TSH is out of the normal range, FT3 and FT4 should be investigated. If the test results of FT3/FT4 cannot be obtained, T3 and T4 can be accepted. If the level of T3/T4 is normal, the patients can be selected.
Urine test: urine protein<2+; if the urine protein≥2+, the 24-hour urine protein quantification must be≤1g;
Echocardiography: LVEF≥55%;
12-lead ECG: Fridericia corrected QTcF<470 msec.
Expected survival time >6 months;
The gene status of KRAS, NRAS, BRAF and HER2 is clear;
Patients are willing and able to follow the protocol during the study, including receiving treatment and scheduled follow-up and examination.
Exclusion Criteria:
Patients will not be accepted into this study if they meet any of the following criteria:
1. History of tumor-related disease and treatment:
2. Co-morbidities and treatment history:
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| Name | Role | Phone | Extension | |
|---|---|---|---|---|
| Xinxiang Li, MD | Contact | +862164175590 | lxx1449@163.com |
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| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Xinxiang Li | Shanghai | Shanghai Municipality | 200032 | China |
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| 5 years after intervention |
| Overall Survival | The time from the beginning of treatment to the date of death. | 5 years after intervention |
| Progression-Free Survival | The time from the start of treatment to PD or death of any cause. | 5 years after intervention |
| Acute toxicity associated with immunotherapy | Proportion of patients with treatment-related acute toxicity. | from the beginning of the treatment to 90 days after the end of immunotherapy |