Ramucirumab for treating advanced gastric cancer or gastro–oesophageal junction adenocarcinoma previously treated with chemotherapy

RAINBOW (Ramucirumab combination therapy)

3.1 RAINBOW was a global, randomised, placebo‑controlled, double‑blind, phase 3 study in which ramucirumab plus paclitaxel was compared with placebo plus paclitaxel. The study, which started in 2010, recruited adults with advanced gastric cancer or gastro–oesophageal junction adenocarcinoma who had disease progression on or within 4 months after treatment with platinum‑containing and fluoropyrimidine‑containing chemotherapeutic regimens with or without an anthracycline.

3.2 The trial randomised 665 adults to have either ramucirumab 8 mg/kg (n=330) or placebo (n=335) intravenously on days 1 and 15, plus paclitaxel 80 mg/m² intravenously on days 1, 8 and 15, over a 28‑day cycle. Randomisation was stratified according to geographic region (region 1 was Europe, Israel, USA and Australia; region 2 was Argentina, Brazil, Chile and Mexico; and region 3 was Hong Kong, Japan, South Korea, Singapore and Taiwan), time to progression from the start of first‑line therapy, and disease measurability. The study was carried out in 170 centres in 27 countries in North and South America, Europe, Asia and Australia.

3.3 People in the trial had metastatic or non‑resectable locally advanced disease, an Eastern Cooperative Oncology Group (ECOG) performance status score of 0 or 1, and adequate haematologic, hepatic, coagulation and renal function. People with squamous cell or undifferentiated gastric cancer were excluded from the trial. People who previously had any chemotherapy other than platinum and fluoropyrimidine, with or without an anthracycline, were also excluded from the trial. Prior treatment with trastuzumab (which has a marketing authorisation in combination with capecitabine or 5‑fluorouracil and cisplatin for HER2‑positive metastatic adenocarcinoma of the stomach or gastro–oesophageal junction, and which has been recommended in NICE's technology appraisal guidance on trastuzumab for the treatment of HER2-positive metastatic gastric cancer as a first‑line treatment) was permitted.

3.4 At baseline, most characteristics were balanced between the treatment groups in RAINBOW. These characteristics included: age; sex; ethnic origin; geographic region; disease measurability; time to progression from the start of first‑line therapy; weight loss in the preceding 3 months; and presence and location of the primary tumour. There was a difference between the treatment groups in ECOG performance status: 35% of people in the ramucirumab plus paclitaxel arm had an ECOG performance score of 0 compared with 43% in the placebo plus paclitaxel arm. A high proportion of people in RAINBOW were male (71%) and most were white (61% white, 35% Asian, 4% black and other). Most people (79%) had gastric cancer and those remaining had gastro–oesophageal junction adenocarcinoma. Previous trastuzumab therapy was had by 20 people in the ramucirumab plus paclitaxel arm compared with 19 people in the placebo plus paclitaxel arm.

3.5 The primary endpoint of RAINBOW was overall survival. Primary and secondary endpoints were analysed using the intention‑to‑treat population (that is, the full population of 665 people who were randomised to the trial). At the date of data cut‑off (12 July 2013), 256 (77.6%) people had died in the ramucirumab plus paclitaxel arm compared with 260 (77.6%) in the placebo plus paclitaxel arm. The data for people who had not died (22.4%) were censored on the last date that the person was known to be alive (on or before the data cut‑off date or lost to follow‑up). Median overall survival was 9.63 months for ramucirumab plus paclitaxel and 7.36 months for placebo plus paclitaxel (2.27‑month improvement in survival; hazard ratio [HR] 0.81; 95% confidence interval [CI] 0.68 to 0.96; p=0.0169). Median progression‑free survival was 4.40 months for ramucirumab plus paclitaxel and 2.86 months for placebo plus paclitaxel (1.54‑month improvement in progression‑free survival; HR 0.64; 95% CI 0.54 to 0.75; p=0.0001).

3.6 Quality of life was assessed in RAINBOW using the European Organisation for Research and Treatment of Cancer (EORTC) QLQ‑C30 (global health status, functioning and symptoms) instrument. Ramucirumab plus paclitaxel was associated with improved outcomes for 14 of the 15 symptom scales compared with placebo plus paclitaxel, although statistical significance was only reached in 2 of the symptom scales: emotional function and nausea and vomiting.

3.7 In RAINBOW, a similar percentage of people in both study arms stopped treatment because of adverse events (11.8% in the ramucirumab plus paclitaxel arm and 11.3% in the placebo plus paclitaxel arm). The most frequently reported treatment‑emergent adverse event was neutropenia, which had a higher all‑grade incidence in the ramucirumab plus paclitaxel arm (54.4%) than the placebo plus paclitaxel arm (31.0%).

Geographic region subgroup results

3.8 The company presented a pre‑specified analysis according to geographic region for RAINBOW. The proportion of people in each geographic region was:

3.9 The company stated that region 1 had characteristics most representative of patients in England. The company presented the outcomes for region 1 showing that in this subgroup there was a 2.66‑month greater median overall survival (p=0.0050), and 1.41‑month greater median progression‑free survival (p<0.0001) for ramucirumab plus paclitaxel compared with placebo plus paclitaxel. The median survival times for both treatment arms in the intention‑to‑treat population of RAINBOW were longer compared with those for region 1, which the company attributed to the higher rates of third- and fourth‑line chemotherapy use among people in region 3 (Asia) after stopping treatment with ramucirumab.

REGARD (ramucirumab monotherapy)

3.10 REGARD was an international, randomised, double‑blind, placebo‑controlled, phase 3 trial in which ramucirumab plus best supportive care was compared with placebo plus best supportive care. The study, which started in 2009, involved adults with advanced gastric cancer or gastro–oesophageal junction adenocarcinoma who had disease progression on or within 4 months after the last dose of treatment with first‑line, platinum‑containing or fluoropyrimidine‑containing chemotherapy, or on or within 6 months after the last dose of adjuvant therapy.

3.11 The trial randomised 355 adults in a 2:1 ratio to have ramucirumab 8 mg/kg (n=238) or placebo (n=117) intravenously once every 2 weeks. Treatment was given until there was evidence of progressive disease or unacceptable toxicity. Randomisation was stratified by geographic region, weight loss over the previous 3 months, and location of the primary tumour (gastric or gastro–oesophageal junction). The study was done across 119 centres in 29 countries in North, Central and South America, Europe, Asia, Australia and Africa.

3.12 People in the trial had metastatic disease or locally recurrent, unresectable disease, a life expectancy of 12 weeks or more, and an ECOG performance status score of 0 or 1.

3.13 The primary endpoint was overall survival. Efficacy analysis was by intention to treat. Median overall survival was 5.2 months for ramucirumab plus best supportive care and 3.8 months for placebo plus best supportive care (1.4‑month improvement in median survival; HR 0.78; 95% CI 0.60 to 1.0; p=0.047). Median progression‑free survival was 2.1 months for ramucirumab plus best supportive care and 1.3 months for placebo plus best supportive care (0.8‑month improvement in median progression-free survival; HR 0.48; 95% CI 0.38 to 0.62; p<0.0001).

3.14 Health-related quality of life in the REGARD trial was assessed using the EORTC‑QLQ‑C30 instrument. At 6 weeks, the proportion of patients with improved or stable quality of life was higher for the ramucirumab arm (34.1%) than the placebo arm (13.7%); but the difference between those people for whom quality‑of‑life data were available was not statistically significant (p=0.23).

3.15 Overall safety results for the REGARD trial showed similar percentages of people in each group had at least 1 serious adverse event: 45% in the ramucirumab group compared with 44% in the placebo group. There was a greater proportion of people who stopped treatment in the ramucirumab group (10.5%) compared with the placebo group (6.0%).

Network meta-analysis

3.16 The company carried out a network meta‑analysis to compare ramucirumab plus paclitaxel with best supportive care and docetaxel. The company identified 23 trials for inclusion in the network, but only 5 trials were included in the analyses of overall survival in the original company submission. The meta‑analysis incorporated evidence for ramucirumab plus paclitaxel (RAINBOW), docetaxel (COUGAR‑02), irinotecan (Hironaka et al. 2013; Roy et al. 2013; Thuss‑Patience et al. 2011), paclitaxel (RAINBOW; Hironaka et al. 2013) and placebo or best supportive care (COUGAR‑02; Thuss‑Patience et al. 2011). Roy et al. (2013) was a non‑randomised multinational study comparing second‑line irinotecan with docetaxel. The company did not include the Roy et al. study to estimate overall survival in the base case, but it did include this study in a sensitivity analysis. It was not the company's preference to include FOLFIRI (a regimen made up of folinic acid, irinotecan and fluorouracil) in the network, but in the company's response to clarification it incorporated FOLFIRI using the trial by Sym et al. (2011).

3.17 Results from the indirect comparison suggested that ramucirumab plus paclitaxel was associated with a statistically significantly improved overall survival compared with best supportive care (HR 0.34; 95% CI 0.17 to 0.71), paclitaxel (HR 0.81; 95% CI 0.68 to 0.96) and irinotecan (HR 0.72; 95% CI 0.52 to 0.99), and with a numerically (but not statistically significant) improved overall survival compared with docetaxel (HR 0.51; 95% CI 0.23 to 1.13) and FOLFIRI (HR 0.86; 95% CI 0.45 to 1.65).

Table 1 Pairwise base‑case results for additional comparators compared with ramucirumab plus paclitaxel using the company's base‑case assumptions*

3.39 The ERG stated that comparing ramucirumab with best supportive care was sufficient. It noted the comparison was in line with the final scope of this guidance, if it is accepted that 'not suitable for paclitaxel' means the same as 'not suitable for further cytotoxic chemotherapy'. If this is not accepted, the ERG stated that comparisons with cytotoxic chemotherapy, other than paclitaxel (docetaxel, irinotecan and FOLFIRI), were missing.

3.40 The ERG stated that, in general, the process for the extrapolation of survival curves was clear; but the choice of the survival modelling did not follow the same procedure for all progression‑free‑survival and overall‑survival curves in the combination‑therapy and monotherapy models. The ERG agreed that for the combination‑therapy model, the Kaplan–Meier overall‑survival curve with exponential extrapolation was the most plausible approach because of the poor fit of parametric functions from independent modelling approaches. The ERG stated that, although it understood the reasons for interval‑censoring adjustments in the modelling for progression‑free survival, this approach appeared to slightly underestimate progression‑free survival for the paclitaxel plus placebo arm to a greater extent than in the ramucirumab plus paclitaxel arm. The ERG also noted that the company had justified using the Weibull‑distribution model because the proportional hazards assumption was held; but it stated that there was evidence suggesting violation such as censoring in the tails, overlapping of Kaplan–Meier curves in the first month and interval censoring. The ERG also noted that the proportional hazards assumption was only assessed between the paclitaxel plus placebo and ramucirumab plus paclitaxel arms; it was assumed to hold for the progression‑free‑survival curves of best supportive care and docetaxel. According to the ERG, choosing the Weibull‑distribution model for progression‑free survival over the log‑logistic (with a better fit) for the sake of the proportional hazards assumption was unnecessary as well as conflicting with the approach taken for modelling overall‑survival curves.

3.41 For the monotherapy model, the ERG commented that it was not clear which approach had been followed in interval-censoring adjustments. In addition, the ERG commented that considering Akaike Information Criteria/Bayesian Information Criteria fit and Cox–Snell residuals, the log‑logistic distribution might have been a more appropriate choice for modelling progression‑free survival, but that the log‑normal and log‑logistic parametric estimates were almost the same. Overall, the ERG concluded that the interval‑censored log‑normal distribution for progression‑free‑survival modelling and the Gamma distribution for overall‑survival modelling were plausible.

3.42 The ERG stated that it would expect the average weight of UK patients to be higher than the RAINBOW baseline patient population (about one‑third of all patients were Asian). The ERG considered it more appropriate to use region 1 data for body surface area and body weight because it is believed that region 1 data better reflected the UK population. The ERG considered the company's scenario analysis in which it adjusted the analysis for region 1 was plausible, but it stated that this was more relevant for body surface area, body weight and hospitalisations. Therefore, the ERG considered that the company's scenario analysis, which only adjusted for overall survival, progression‑free survival and time on treatment, was not appropriate as a new base case.

3.43 The ERG commented that using an incidence‑based threshold criterion (5% in each relevant treatment arm) for the inclusion of adverse events resulted in a different selection of adverse events for best supportive care in the combination‑therapy and monotherapy models. According to the ERG, this approach was inconsistent.

3.44 The ERG indicated a potential double counting of hospitalisation costs because Health Resource Groups' (HRGs) codes referring to adverse events also take hospitalisations into account. In the response to the clarification letter, the company provided a scenario that reduced the rate of hospitalisations by an estimate of the proportion of hospitalisations due to adverse events. The ERG used these adjusted hospitalisation rates in its exploratory analyses for its base case. The ERG found an error in the half‑cycle correction of the model submitted by the company. The impact of this correction on the ICER was negligible. The ERG also found a technical error in the costs for docetaxel (both in the second and third line). Furthermore, according to the ERG, the drug acquisition costs for ramucirumab plus paclitaxel were underestimated because these were based on the average weight of the patients in the RAINBOW trial (one‑third of patients in RAINBOW were Asian).

3.45 The ERG did an exploratory analysis and in its base case it included the following adjustments:

3.46 The ERG analysis resulted in ICERs compared with best supportive care of £129,431 and £188,055 per QALY gained for the combination‑therapy and monotherapy models respectively. For the combination therapy model, the ERG also applied these amendments to analyses in which the comparator was first, docetaxel, and second, paclitaxel. When the comparator treatment was docetaxel, the ICER increased to £168,164 per QALY gained. When the comparator treatment was paclitaxel, the ICER increased substantially to £359,794 per QALY gained. In both of these analyses, the increase in the ICER was largely due to removing the double counting of hospitalisations for adverse events and using body surface or weight based on region 1. However, the increase was much greater when the comparator was paclitaxel. This was because the impact on the costs of docetaxel when the body surface area was based on region 1 was much lower than for ramucirumab and paclitaxel.

3.47 In addition, the ERG explored 3 different scenarios in the combination‑therapy model: