The protocol has been structured according to the Standard Protocol Items: Recommendations for Interventional Trials (SPIRIT 2013 Checklist) (Appendix S1).
Study setting
This study is a prospective, single-centre, randomized, double-blind controlled study in which 300 patients will be randomly assigned to the test group or the control group in a 1:1 allocation ratio. The study protocol can be accessed at the chictr.org.cn website (ChiCTR2100046201). figure 1 shows the trial flow chart.
Eligibility criteria
1. Patients who meet any of the following conditions will be included:
1) Patients of both sexes between 18- and 80-years-old;
2) Colon cancer (ct3-4an0-3m0 [UICC/ajcc-8th Colon Cancer TNM tumour stage]), rectal cancer (ct3-4n0-3m0 or any CT/N + [UICC/ajcc-8th Rectal Cancer TNM tumour stage]) and patients diagnosed and treated directly with surgery at each study centre;
3) Patients who voluntarily agreed to join this study and signed the relevant informed consent form after verbal discussion about the clinical trial and discussion of the intention of obtaining informed consent.
2. Patients who meet any of the following conditions will be excluded:
1) Taking various classes of antibiotic medications on their own or with medical advice for various reasons within 2 weeks before surgery;
2) Previous diagnosis or current diagnosis of inflammatory bowel disease;
3) Diagnosed with acute intestinal perforation or acute small intestinal diverticulum;
4) Those with ischaemic colitis or infectious colitis were included in the diagnosis
5) Diagnostic finding of other comorbid local or systemic disease that requires anti-infective treatment;
6) Two and more simultaneous surgeries;
7) Had been diagnosed due to acute and chronic peritonitis or other infectious diseases that require anti-infective treatment in the perioperative period;
8) Any acute physiological disturbance that indicates that the subject requires emergency surgery without elective surgery [e.g.: need for preoperative mechanical ventilation, preoperative acute renal failure, preoperative systemic inflammatory release syndrome, sepsis or septic shock, etc.];
9) ASA was rated on a 5-level scale;
10) Immunodeficiency, immunosuppression or autoimmune diseases (e.g., allogeneic bone marrow transplant patients within the last five years, taking immunosuppressive drugs, SLE, etc.);
11) The subject refused to sign an informed consent form to participate in the trial;
12) Other scenarios in which normal cooperation with a physician was not possible for personal reasons or the investigator considered it unsuitable to participate in the experiment;
13) All single port laparoscopic procedures, transhiatal procedures, and various new surgical modalities need to be used;
3. The terminating study criteria are as follows:
1) Subject's violation of treatment principles after enrolment (such as violation of entry criteria, noncompliance with study treatment medication or surgical arrangements);
2) Subject was inoperable for various reasons after enrolment (reasons to be recorded);
3) Subjects had nonstudy-related complications, such as drug hypersensitivity reactions, after enrolment;
4) Because of the occurrence of adverse events, after the judgement of the investigator, the subject was not considered suitable to continue with the trial (the reason for withdrawal was recorded);
5) Subjects or the subject's legally authorized representative required withdrawal from the study;
6) Subjects developed serious complications or intolerable adverse reactions;
7) The subject was not available for elective surgery after enrolment due to exacerbation of intercurrent illness or other reasons;
Interventions
Metronidazole/placebo: Treatment regimens were developed on their own according to each centre’s metronidazole specifications, which required maintenance of metronidazole plasma concentrations for subjects in the experimental group to be > 0.01 μG/ml, and the duration of administration was tentatively set at five years (i.e., the time of the outcome of this experiment).
The chemotherapy regimen is eFOLFOX6:
Oxaliplatin 85 mg/m2 IV infusion for 2 hours, D1; Leucovorin 400 mg/m2 IV for 2 hours, D1; Fluorouracil 400 mg/m2 IV bolus on D1 followed by 1200 mg/m2/DX2 continuous IV infusion (total 2400 mg/m2 over 46-48 hours infusion). This process was repeated every 2 weeks for a total of 24 weeks. (table 1)
Outcomes
Primary outcome
Efficacy will be measured in terms of the incidence of postoperative liver metastasis within 5 years after surgery.
Assessment will be conducted by in-person visits; should the status of the pandemic impact the study with no possibility of performing in-person 5-year follow-up appointments, telemonitoring might be considered using validated tools.
Considering that the dose of metronidazole is predicted in the form of hypothesis, the incidence of drug-related adverse events will be regarded as one of the main indicators of this study.
Secondary outcomes
1. Postoperative complication rates: Postoperative complications will be classified according to their impact and the required management (e.g., medical treatment, reoperation, drainage), as proposed by Clavien–Dindo.
Complications will be assessed at the 30-day follow-up; ancillary studies will assess complications at the 60-day and 5-year follow-ups. The Cumulative Complication Index will also be computed to assess the global burden of complications on each patient.
2. Complete postoperative recovery: number of days between admission and when the patient is suitable for discharge.
3. Unplanned secondary surgery
4. Readmission: need for any unplanned readmission after discharge for any reason.
5. 1-year, 3-year and 5-year survival rates
6. Relapse-Free Survival (RFS)
7. Overall survival (OS)
Randomization/assignment of interventions
Randomization was stratified by centre. Once informed consent is obtained, randomization will be performed via a centrally managed database. After receiving the patient grouping information, designated researchers will prepare trial drugs or placebo for patients according to the assigned group. In this process, only the researchers are informed about the grouping of patients. They will sign a confidentiality agreement and will not participate in any other links of the trial to ensure that they will not have any impact on the study. After collecting all the data, the designated researcher named the two Groups A and B. The analyst will analyse the primary and secondary results without knowing the group name. Only after the analysis of the primary and secondary results can complete blindness be eliminated and ineffective blinding events recorded (for example, the study nurse discloses the patient's specific medication to the doctor).
The nurses provided the patients with oral antibiotics for the experimental group and placebo for the control group in the ward.
Allocation concealment mechanism
The randomization was performed on a centrally managed database once informed consent was obtained.
Implementation
The sequence will be generated and forwarded by the computer specialist who created the case report form (CRF) online to implement the online database. By doing so, each investigator can randomize their patients and assign them to the respective group of treatments. The date of randomization will be recorded.
Blinding (masking)
The blind level was set as double-blind. All patients, doctors, data collectors and analysts will be unaware of the grouping of patients.
Data collection, management, and analysis
Clinical data
Clinical data from patients will be obtained by medical staff and recorded on an online electronic platform (Http://www.medresman.org.cn) and in the CRF table. The sample will be coded, and the patient's identity will be known only by the attending physician. The clinical data will include the following: general patient information, past medical history, past surgical history, laboratory examination results, imaging results, surgery details, postoperative infection rate, incidence of postoperative complications, incidence of anastomotic leakage, and 30-day readmission rate after surgery. The timing and processing of the above recorded contents will all be reflected in the CRF table, and the laboratory examinations will mainly assess preoperative and postoperative routine blood and inflammatory indicators. (table 2)
A detailed description of the above data is shown in the CRF table.
Sample size calculation basis and formula
A larger sample size is required for this study to provide adequate statistical power.
Based on our current known information and two similar clinical studies on recurrence and metastasis of colorectal cancer (1108 patients enrolled in a berberine hydrochloride clinical trial for colorectal adenoma prevention by Ying Xuan Chen et al., Shanghai Renji Hospital, 2014-2016, Lei Huang et al. from the First Affiliated Hospital of Anhui Medical University during the 2015-2020 clinical trial of aspirin to prevent colorectal cancer metastasis were planned to enrol 3000 patients) and combined with feasibility and study length consideration, we determined the sample size to be 300 patients, experimental group: control group = 1:1, that is, 150 patients in the experimental group and 150 patients in the control group.
Statistical analysis
The association with the variables of interest will be compared between groups by means of Pearson's chi-squared test or Fisher's exact test, as appropriate and in the case of categorical variables. For continuous variables, Student’s t test for independent samples and the Mann–Whitney U test will be used for normally and nonnormally distributed variables, respectively.
The analysis for the primary end-point variable (incidence of postoperative liver metastasis) will be performed with an intention-to-treat approach. The absolute difference in terms of incidence will be computed, along with 95% confidence intervals, and will be expressed as relative risk or odds ratio, as appropriate for each outcome.
An interim analysis is planned, once 50% of the patients have completed their treatment (half of the patients per arm). The study can be suspended if the treatment superiority is statistically significant, with a P value set at <0.0052. The interim analysis will be performed in agreement with previously reported epidemiological and statistical criteria.
For the secondary variables, a similar approach will be used, using the effect estimate with a 95% confidence interval and the relative risk and odds ratio for categorical variables.
Any potential effects related to centres or surgeons will be assessed by means of mixed models. For the primary end-point variable, a bivariate and multivariate analysis will be performed to identify the potential effects of other variables.
The value for statistical significance at final analysis was set at P < 0.05. Statistical analysis will be performed with SPSS 20. All the deviations from the original statistical plan will be described and justified. All subjects included in the study will be included in the analysis.
Safety
Adverse events refer to adverse medical events that occur in clinical trial patients after receiving medications. In this study, an adverse event will be considered regardless of whether it is related to the therapy from the time when patients sign the informed consent form to 1 month after the end of treatment. Assessing the nature and determining the severity of adverse events will be conducted in accordance with “expert consensus on diagnostic criteria for postoperative complications of gastrointestinal cancer in China”. To assess the adverse events and their causal relationship to therapy, the investigator will evaluate the possible associations between adverse events and trial medications. The following five criteria will be used to determine the results: the time of occurrence of adverse events coincides with the time of administration, adverse events are related to known adverse reactions of the medication, adverse events cannot be explained by other reasons, adverse events disappear after discontinuing therapy and adverse events are reproduced after medication administration. The results documented as positive, relevant and possibly related were deemed to be adverse reactions. The incidence of adverse reactions will be calculated accordingly. To record, process and report adverse events, the investigator will document any adverse events. Records of adverse events will include a description of adverse events and all related symptoms, time of occurrence, severity, duration, measures taken, the results and final outcomes. The reporting methods and treatment measures for severe adverse events will be classified as severe adverse events if they meet one or more of the following criteria: death, life-threatening (e.g., immediate risk of death), prolonged hospitalization or hospitalization, permanent or severe disability, congenital malformations or defects, some events that have not yet caused death, danger to life or hospitalization but will consider a severe adverse event by a physician if they cause harm to the patient or require medication or surgical treatment to avoid the above situation. For any severe adverse events during the clinical trial, the investigator will file a report of severe adverse events within 24 hours and report in writing to the Ethics Committee, the superior authorities and the sponsor. The written report will include the time, severity, duration, measures taken and outcomes of serious adverse events.
Patient protection/written informed consent forms
Both parties ensure the protection of the patient's personal records. Except for documents required by law, patient names are not included in any form in tabular reports, publications, or any type of research publication document. Informed consent will be formulated in strict accordance with Chinese laws and regulations. Written informed consent, including all changes made throughout the study, must be preapproved by the Internal Review Board/Independent Ethics Committee before inclusion in the study. Medical staff at each centre will obtain a signature with written informed consent from each patient (if the patient is unable to make their own decision for various reasons, the immediate family will decide on their behalf) prior to any specific activities related to the study. Researchers at each centre will submit and keep original copies of all written informed consent forms signed by patients and provide additional copies to patients or their immediate family members for their records.
Monitoring
Data monitoring
The investigators will not have access to data until the study is completed and data are analysed. A data monitoring committee is established at Xijing Hospital, which will assess the results and safety of the treatments performed at all centres.
Representatives authorized by project undertakers, regulatory departments, and independent ethics committees may visit the centre for inspections, including verifying the original data every year. The purpose of the inspections of the site and personnel is to systematically and independently examine all research-related behaviours and documents, to determine that these behaviours have been managed and that the data have been analysed, recorded and accurately reported in accordance with the research programme, GCP, ICH guidelines and other regulatory requirements.
During the study period, the project undertaker or the supervisor representing the project will regularly contact the research centre for a number of reasons including the following: providing information and technical support; establishing randomized grouping as required; confirming that the investigator complies with the study plan, that data on the CRFs are accurately recorded, and that dosage of drugs being used is checked; and carrying out original data analysis (e.g., the data on CRFs are related to the records of patients in the hospital, and the research will compare these with other records). This requires direct access to the original records of each patient (e.g., clinical charts).
Auditing
Every 3 months and at the time of interim analysis (performed once 50% of the planned sample of patients completed the primary endpoint follow-up), the data monitoring committee examined the data to verify the safety of treatment in both arms.
Data ascertainment
For case ascertainment, a screening log will be used, where the following data will be collected:
1. eligible patients according to the eligibility criteria;
2. patients who were asked for consent;
3. patients who agreed to enter the study.
Patient protection/written informed consent forms
Both parties ensure the protection of the patient's personal records. Except for documents required by law, patient names are not included in any form in tabular reports, publications or any type of research publication document. Informed consent will be formulated in strict accordance with Chinese laws and regulations. Written informed consent, including all changes made throughout the study, must be preapproved by the Internal Review Board/Independent Ethics Committee before inclusion in the study. Medical staff will obtain a signature with written informed consent from each patient (if the patient is unable to make their own decision for various reasons, the immediate family will decide on their behalf) prior to any specific activities related to the study. Researchers will keep original copies of all written informed consent forms signed by patients and provide additional copies to patients or their immediate family members for their records.