FOXFIRE protocol: an open-label, randomised, phase III trial of 5-fluorouracil, oxaliplatin and folinic acid (OxMdG) with or without interventional Selective Internal Radiation Therapy (SIRT) as first-line treatment for patients with unresectable liver-only or liver-dominant metastatic colorectal cancer

The FOXFIRE trial is a phase III, open label, multicentre, parallel two-arm, randomised controlled trial of OxMdG chemotherapy with or without the addition of interventional SIRT for patients with liver-only or liver-dominant mCRC. Patients will be recruited at 34 UK centres with 20 being specialist SIRT centres and the remaining being chemotherapy-only centres feeding into pre-specified SIRT centres. Prior to site activation, all SIRT centres will have treated at least three patients with SIRT to demonstrate that they have adequate training, support and mentoring in place to perform the treatment safely. Eligible patients are randomised 1:1 to receive either systemic chemotherapy with oxaliplatin, 5-fluorouracil and folic acid (OxMdG) or single-session whole liver SIRT + OxMdG (Figure 1).

Following consent, eligible patients will be randomised 1:1 to OxMdG ± SIRT using a central computer system. Simple randomisation is used for the first 30 patients followed by minimisation with a random element (0.8) [12] and using the stratification factors: presence or absence of extra-hepatic metastases, extent of tumour involvement of the liver (≤25% or >25% tumour involvement determined by computed tomography [CT] scan), investigational centre, and intention to treat with a biological agent (introduced in March 2011 following a shift in the international standard treatment paradigm for these patients).

Systemic chemotherapy must start within 28 days of randomisation. In the control arm, systematic chemotherapy with OxMdG consists of oxaliplatin (85 mg/m² infusion over 2 hours), folinic acid (l-folinic acid 175 mg or d, l-folinic acid 350 mg infusion over 2 hours) and 5-FU (400 mg/m² bolus followed by a 2400 mg/m² continuous infusion over 46 hours). This cycle is then repeated every 14 days for 12 cycles. In the treatment arm, SIRT is administered on the third or fourth day of the second chemotherapy cycle. In addition, the same chemotherapy regimen is used except in cycles 2–4 when the oxaliplatin dose was reduced to 60 mg/m² as this has been demonstrated as the maximum tolerated dose in an earlier phase I-II trial [11]. SIRT requires a hepatic arteriogram and a liver-to-lung breakthrough nuclear medicine scan to ensure suitability for receiving this procedure, and to plan the delivery of the SIR-spheres. A separate SIR-Spheres users’ manual details the technique for delivery of the SIR-Spheres. The prescribed activity of SIR-Spheres will be determined from the patient’s body surface area (BSA), the percentage tumour involvement, and the magnitude of liver-to-lung shunting. The dosing charts used are consistent with a similar contemporary study (SIRFLOX study protocol, submitted to BMC Cancer, March 2014).

The use of a licensed biological agent (e.g. cetuximab, bevacizumab) is permitted in this trial at the discretion of the treating investigator and at doses determined by local practice, but the intention to treat a patient with a biological agent should be declared at the time of randomisation. Intention to treat with a biological agent is a stratification factor in the trial. The biological agent can be added at any time during protocol chemotherapy for patients randomised to chemotherapy only, but, on account of a potential interaction with liver radiotherapy, it should not be delivered prior to cycle 7 for patients randomised to receive SIRT.

Once protocol treatment is completed, patients should be given the best available care based upon clinical assessment and patient preference. In both arms, if following treatment response the patient is deemed a candidate for surgical resection (assessed at 3 and 6 months after starting protocol treatment), and the patient undergoes surgical resection and/or complete ablation of their primary and metastatic cancer, protocol OxMdG chemotherapy should be continued as scheduled if appropriate.

The primary endpoint of the FOXFIRE trial is a comparison of OS between treatment arms. Secondary endpoints include safety, progression-free survival (PFS), liver-specific PFS, response and resection rate, time until next therapy, patient-reported outcomes (PROs) and cost-effectiveness. All patients will be assessed by the criteria.

OS is defined as the time from randomisation until death from any cause with patients censored at the last date alive if they are not known to have died by the end of the follow-up period. PFS is defined as the time from randomisation until disease progression (RECIST version 1.1 guidelines [13]) or death from any cause with censoring at the last date alive and progression-free. PFS and response rate will be determined from serial CT scans. Sample scans are being collected from each centre for central review as part of radiology quality assurance.

Liver-specific PFS is defined as for PFS but until documented progression in the liver. Adverse events (AEs) and Serious Adverse Events (SAEs) will be collected and rated according to Common Terminology Criteria for Adverse Events (CTCAE) v3.0 and the relationship to protocol therapy will be rated as none, unlikely, possible or probable.

PROs are assessed using the generic EORTC Quality of Life Questionnaire (QLQ-C30) and disease specific EORTC QLQ-LMC21 with pre-specified outcomes of global quality of life at 12 months and fatigue at cycle 4. Health economic outcomes will be based upon the quality of life measured by EQ-5D and collection of health economic data including costs of chemotherapy and SIRT (including the use of ancillary services and treatments), hospital visits, imaging, surgical procedures, and in-patient lengths of stay.

It was originally planned to recruit this number of patients from both FOXFIRE (n = 490) and SIRFLOX (n = 320) and carry out a combined analysis for OS. Following changes to the treatment paradigm in liver metastatic colorectal cancer SIRFLOX allowed the use of bevacizumab in suitable patients and the intention-to-treat with bevacizumab was included as a stratification factor. FOXFIRE also allowed appropriate treatment with a biological agent, including bevacizumab and cetuximab, adding intention-to-treat with a biological agent as a stratification factor. The use of biological agents will potentially prolong the PFS time and this has led to increasing the sample size for PFS in SIRFLOX. Thus, the overall sample size for the combined endpoint has been adjusted to take into account changes in the expected median OS for the control group. We therefore predict that 1022 patients will be required to observe the 631 events required to detect a hazard ratio of 0.8 with 80% power and two-sided 5% significance. This number of patients will include at least 320 patients recruited in FOXFIRE, 500 patients recruited in SIRFLOX and the additional patients being recruited into an extension study to SIRFLOX, called FOXFIRE-Global. It is anticipated that the required number of participants will have been recruited by October 2014.

All analyses will be conducted on an intention-to-treat (ITT) basis. The primary endpoint of OS will be analysed after all patients recruited into FOXFIRE and SIRFLOX have been followed up for at least 2 years and at least 631 deaths have been observed. Analysis will be by Kaplan-Meier survival curves and unadjusted log-rank test. The primary analysis will be a two-stage meta-analysis of individual patient data with the first stage consisting of within trial analyses and the second stage being a pooled analysis of the separate within trial analysis results. A secondary analysis will be undertaken using the one-stage approach also using individual patient data but for all patients, in order to investigate other aspects of the trial and covariates. Response and resection rates will be compared using test of proportions and the unadjusted log rank test will be used to compare time to event endpoints. PROs will be compared using ANCOVA adjusting for baseline values, with pre-specified variables compared using 5% (2-sided) significance and the other functional and symptom scales assessed using 1% (2-sided) significance.

Sensitivity analyses will be performed adjusting for minimisation and prognostic factors and by trial (FOXFIRE/SIRFLOX) in a multivariate analysis framework. This includes the impact of explanatory variables on various outcome measures of interest. Proportional hazards regression will be used to model time to event outcomes, multiple linear regression to model continuous outcomes (with appropriate transformations if necessary) such as the PROs, logistic regression to model binary outcomes (such as response) and ordered logistic regression for ordered categorical outcomes (such as toxicity grades).

The Data and Safety Monitoring Committee (DSMC) will review the results from several interim analyses using data from both the FOXFIRE and SIRFLOX trials, these include: analysis of toxicity and safety approximately 8 months after at least 80 patients are randomised (a minimum of 40 patients per trial); and analysis of toxicity and safety approximately 8 months after at least 300 patients are randomised (a minimum of 120 patients per trial). Further specifics of all analyses will be agreed with the DSMC and included in the statistical analysis plan.