Abstract
Pemetrexed, a multitargeting antifolate cytotoxic drug, plays a leading role in front-line chemotherapy for patients with advanced non-squamous non-small-cell lung cancer (NSCLC). Following its approval as second-line monotherapy for locally advanced or metastatic non-squamous NSCLC, pemetrexed has established itself as the first-line regimen in combination with cisplatin, and its powerful antitumor effects and less cumulative toxicities were then taken advantage of in the JMEN and PARAMOUNT trials, respectively, to pioneer a new treatment strategy of switch and continuation maintenance monotherapy. These developments have brought about a marked paradigm shift, and made pemetrexed indispensable in the treatment for non-squamous NSCLC. So far, only three drugs have been approved for maintenance therapy; pemetrexed both by switch and continuation maintenance, erlotinib by switch maintenance, and bevacizumab by continuation maintenance. Compared with observation alone after defined cycles of the first-line chemotherapy, subsequent pemetrexed maintenance therapy has provided significantly longer survival and infrequent severe adverse events. The cost-effectiveness of pemetrexed maintenance therapy is controversial, as well as the other two maintenance drugs, bevacizumab and erlotinib. The latest attractive attention is a combination maintenance therapy. We may have to consider epidermal growth factor receptor (EGFR) mutation status for selection of a combination pattern. A combination maintenance therapy of pemetrexed plus bevacizumab is potential for patients with wild-type EGFR status, while a EGFR tyrosine kinase inhibitor-containing combination is promising for patients with active EGFR mutation status. Pemetrexed will be a pivotal drug when a combination maintenance therapy is used in practice. For future maintenance therapy, we need to explore reliable predictive selection or exclusion markers that can predict who will really benefit from maintenance therapy.
Keywords: pemetrexed, maintenance therapy, continuation, switch, non-squamous non-small cell carcinoma, cost-effectiveness, epidermal growth factor mutation
Introduction
Lung cancer is a leading cause of cancer mortality and accounted for 1.59 deaths worldwide in 2012.1 Histopathologically, lung cancer is divided broadly into two groups, ie, non-small-cell lung cancer (NSCLC) and small cell lung cancer. The former accounts for 80%–85% of all lung cancer cases, and is further divided into several subgroups, ie, adenocarcinoma, squamous cell carcinoma, large cell carcinoma, and others. Most patients with NSCLC are diagnosed when their disease has already advanced locally or metastasized systemically. For inoperable patients with good performance status, chemotherapy is a standard treatment option.
Pemetrexed (Alimta®, Eli Lilly, Indianapolis, IN, USA) is a multitargeted antifolate drug that inhibits replication and survival of cancer cells by disrupting folate-dependent metabolic processes. During the past decade, this drug has come to have a leading role in front-line chemotherapy for patients with advanced non-squamous NSCLC, owing to its antitumor effects and mild toxicity.
When combined with platinum in a first-line regimen for non-squamous NSCLC, pemetrexed is superior or similar in efficacy and superior in toxicities to other third-generation antitumor drugs. There were three randomized Phase III studies that compared various endpoints between platinum plus pemetrexed and conventional platinum-based doublets in NSCLC (Table 1).2–4 Among them, a milestone was the JMDB trial,4 in which cisplatin plus pemetrexed showed non-inferiority in overall survival (OS) and better tolerability compared with cisplatin plus gemcitabine. In addition, this trial also indicated a histological difference in efficacy. Namely, pemetrexed improved OS for patients with non-squamous histology, but failed for patients with squamous histology. These results led to the approval of cisplatin plus pemetrexed for patients with advanced non-squamous NSCLC as a first-line regimen by the European Medicines Agency in April 2008 and by the US Food and Drug Administration in September 2008. Health-related quality of life and survival without grade 3 or 4 toxicity (SWT) was compared between carboplatin plus pemetrexed and carboplatin plus gemcitabine in a Norwegian study and between carboplatin plus pemetrexed and carboplatin plus docetaxel in a multinational study, respectively.2,3 Compared with control regimens, carboplatin plus pemetrexed provided similar health-related quality of life and OS in the Norwegian study,2 and longer SWT but similar OS in the other study.3 In addition, platinum plus pemetrexed was generally less toxic, except for severe nausea,4 and generally caused less frequent severe leukopenia and neutropenia than control regimens in all studies (Table 2).2–4
Table 1.
Phase III studies of combinations of pemetrexed plus platinum compared with standard platinum-based doublets
| Reference | Primary endpoint | n | Regimens | RR (%) | PFS (M) | HR P-value |
OS (M) | HR P-value |
|---|---|---|---|---|---|---|---|---|
| Scagliottii et al4 (JMDB trial) | OSa | All NSCLC, entire population | ||||||
| 862 | CDDP + PEM | 30.6 | 4.8 | HR 1.04 | 10.3 | HR 0.94 | ||
| 863 | CDDP + GEM ×6 cycles | 28.2 | 5.1 | Non-inferior | 10.3 | Non-inferior | ||
| Non-SQ NSCLC subgroup | ||||||||
| 512 | CDDP + PEM | ND | 5.3 | HR 0.90 | 11.8 | HR 0.81 | ||
| 488 | CDDP + GEM | ND | 4.7 | ND | 10.4 | P=0.005 | ||
| Grønberg et al2 | HRQoLb | All NSCLC, entire population | ||||||
| 225 | CBDCA + PEM | ND | ND | ND | 7.3 | HR ND | ||
| 221 | CBDCA + GEM ×4 cycles | ND | ND | ND | 7.0 | P=0.63 | ||
| Non-SQ NSCLC subgroup | ||||||||
| 127 | CBDCA + PEM | ND | ND | ND | 7.8 | HR ND | ||
| 121 | CBDCA + GEM | ND | ND | ND | 7.5 | P=0.77 | ||
| Rodrigues-Pereira et al3 | SWT | All non-SQ NSCLC | ||||||
| 128 | CBDCA + PEM | 34.0 | 5.8 | HR 0.91 | 14.9 | HR 0.93 | ||
| 132 | CBDCA + DTX ×6 cycles | 22.9 | 6.0 | P=0.534 | 14.7 | P=0.698 | ||
| SWT | ||||||||
| 128 | CBDCA + PEM | 3.2 | HR 0.45 | |||||
| 132 | CBDCA + DTX | 0.7 | P<0.001 | |||||
Notes:
Non-inferiority design;
defined as the four clinically relevant domains of global quality of life, nausea/vomiting, dyspnea and fatigue, and assessed by the European Organisation for Research and Treatment of Cancer Quality of Life Questionnaire C30 (QLQ-C30) and the lung cancer–specific module LC13 during the first 20 weeks.
Abbreviations: CBDCA, carboplatin; CDDP, cisplatin; DTX, docetaxel; GEM, gemcitabine; HR, hazard ratio; HRQoL, health-related quality of life; M, months; ND, not described; RR, response rate; OS, overall survival; PEM, pemetrexed; PFS, progression-free survival; SQ, squamous cell carcinoma; SWT, survival without treatment-emergent grade 3/4 toxicity.
Table 2.
Comparison of statistically significant adverse effects between pemetrexed-containing and control regimens
| Reference
|
Scagliotti et al4 (JMDB trial) |
Grønberg et al2
|
Rodrigues-Pereira et al3
|
|||
|---|---|---|---|---|---|---|
| Regimens | CDDP + PEM | CDDP + GEM | CBDCA + PEM | CBDCA + GEM | CBDCA + PEM | CBDCA + DTX |
| n | 839 | 830 | 219 | 217 | 106 | 105 |
| Hematologic | ||||||
| Leukopenia, grade 3–4 (%) | 4.8a | 7.6 | 23a | 46 | 16.0a | 40.0 |
| Neutropenia, grade 3–4 (%) | 15.1a | 26.7 | 40a | 51 | 33.0a | 64.8 |
| Anemia, grade 3–4 (%) | 5.6a | 9.9 | 13 | 13 | 12.3a | 1.9 |
| Thrombocytopenia, grade 3–4 (%) | 4.1a | 12.7 | 24a | 56 | 9.4 | 2.9 |
| Non-hematologic | ||||||
| Febrile neutropenia, grade 3–4 (%) | 1.3a | 3.7 | ND | ND | 0a | 8.9 |
| Alopecia, any grade (%) | 11.9a | 21.4 | ND | ND | 8.5a | 42.9 |
| Nausea, grade 3–4 (%) | 7.2a | 3.9 | 3 | 4 | 0.9 | 1.0 |
| Diarrhea, any grade (%) | ND | ND | ND | ND | 6.6a | 20.0 |
| Abdominal pain, any grade (%) | ND | ND | ND | ND | 1.9a | 9.5 |
Note:
Statistically significant (P<0.05).
Abbreviations: CBDCA, carboplatin; CDDP, cisplatin; DTX, docetaxel; GEM, gemcitabine; ND, not described; PEM, pemetrexed.
Concerning cost-effectiveness, the platinum plus pemetrexed doublet is considered to be cost-effective, particularly in patients with non-squamous NSCLC histology (Table 3). There were two US studies with different approaches for first-line platinum plus pemetrexed.5,6 Based on a state transition model, Klein et al concluded that cisplatin plus pemetrexed was a cost-effective treatment for patients with non-squamous NSCLC when compared with cisplatin plus gemcitabine and a commonly mentioned but unwarranted threshold of US $100,000 per life-year gained (LYG) in the USA.5 Compared with a first-line combination of cisplatin plus gemcitabine, cisplatin plus pemetrexed led to an incremental cost per LYG of US $104,577 for patients with NSCLC regardless of histological subtype, but a cost of US $83,537 for patients with non-squamous NSCLC. Thus, considering the effect of prolongation of survival by the pemetrexed-containing regimen, pemetrexed was expensive but within the allowance. Based on indirect comparisons of the following three regimens in different studies because of no available head-to-head data, platinum plus pemetrexed was also considered more cost-effective than a triplet of bevacizumab combined with carboplatin plus paclitaxel, but controversial when compared with a doublet of carboplatin plus paclitaxel, as the pemetrexed-containing regimen was more costly but more effective than carboplatin plus paclitaxel.5,6 In September 2009, the National Institute for Health and Clinical Excellence (NICE) in the UK recommended pemetrexed in combination with cisplatin as an option for the first-line treatment of patients with non-squamous NSCLC, using the single technology appraisal process and based on the Evidence Review Group’s exploratory analysis indicating that the incremental cost-effectiveness ratios (ICERs) for cisplatin plus pemetrexed compared with cisplatin plus gemcitabine were between £20,000 and £30,000 per quality-adjusted life-year (QALY) gained for non-squamous NSCLC and between £17,000 and £25,000 per QALY for adenocarcinoma or large-cell carcinoma, all under the willing-to-pay threshold of £30,000 per QALY gained.7
Table 3.
Comparison in cost-effectiveness of direct medical costs between first-line pemetrexed-containing regimen with another platinum-doublet regimen: study deigns and results (monetary unit, US $)
| Reference | Methods, cost and outcome discount, study perspective, time frame | Data sources | Study population | Regimen | Histology | Cost | LYG or OSa | QALY | ICERa / LYG | ICER / QALY |
|---|---|---|---|---|---|---|---|---|---|---|
| Klein et al5 (US) | Semi-Markov model No discount U.S. payer’s perspective Time frame; 2 year | Clinical parameters; RCT (JMDB) Cost; Medicare reimbursement rates and average doses, PharMetrics claim database | Chemotherapy-naïve, stage IIIB/IV, non-SQ or all histology NSCLC, BSA 1.8 m2 | CDDP + PEM | Non-SQ | $ 65,517 | 0.9652 Y | 0.5016 | ||
| All NSCLC | $ 66,606 | 0.9587 Y | 0.4943 | |||||||
| CDDP + GEM | ||||||||||
| Incremental CDDP +PEM to CDDP+GEM | ||||||||||
| Non-SQ | $ 61,008 | 0.9112 Y | 0.4676 | $ 83,537 | $ 132,829 | |||||
| All NSCLC | $ 61,535 | 0.9102 Y | 0.4661 | $ 104,577 | $ 179,597 | |||||
| CBDCA + PTX | ||||||||||
| Incremental CDDP +PEM to CBDCA+PTX | ||||||||||
| Non-SQ | $ 52,885 | 0.8945 Y | 0.4513 | $ 178,613 | $ 250,992 | |||||
| All NSCLC | $ 50,283 | 0.8882 Y | 0.4469 | $ 231,291 | $ 343,870 | |||||
| CBDCA + PTX + Bev → Bev maintenance (Bev 15 mg/kg) | ||||||||||
| Incremental CBDCA +PTX +Bev→Bev to CDDP+PEM | ||||||||||
| Non-SQ | $ 90,044 | 1.0379 Y | 0.5260 | $ 337,179 | $ 1,006,065 | |||||
| Shah et al6 (US) | Retrospective cohort study of real world data documented in PMS data Time frame; 1 year | ION clinical oncology database, PMS data, SSA’s Death Index Master file | First-line treatment between 2006 and 2009, advanced non-SQ NSCLC | Platinum + PEM | Non-SQ | $ 33,969 | 190 days | ND | ||
| CBDCA + PTX | ||||||||||
| Incremental CBDCA+PTX to Platinum+PEM for OS | ||||||||||
| $14,832 | 132 days | ND | $ 330 | ND | ||||||
| CBDCA + PTX + Bev → Bev maintenance | ||||||||||
| Incremental CBDCA +PTX+Bev→Bev to Platinum +PE M for OS | ||||||||||
| $ 53,915 | 163 days | ND | -$ 739 | ND | ||||||
Notes:
Studies by Klein et al and by Shah et al presented LYG (years) and OS (days), ICER (cost / LYG, US $) and mean incremental cost/day (US $), respectively.
Abbreviations: BSA, body surface area; Bev, bevacizumab; CBDCA, carboplatin; CDDP, cisplatin; ICER, incremental cost-effectiveness ratio; ION, International Oncology Network; LYG, life-year gained; ND, not described; NSCLC, non-small cell lung cancer; OS, overall survival; PEM, pemetrexed; PTX, paclitaxel; QALY, quality-adjusted life-year; SQ, squamous cell carcinoma; RCT, randomized controlled trial; PMS, practice management system; SSA, Social Security Administration; Y, years.
Options for maintenance therapy; continuation maintenance versus switch maintenance
Maintenance therapy after 4–6 cycles of platinum-based induction chemotherapy is a standard first-line regimen for patients with advanced non-squamous NSCLC. Maintenance therapies are classified broadly into two types, ie, continuation maintenance and switch maintenance. The former is a continuation of one or two drugs used in the induction regimen and the latter involves introduction of an additional drug that was not used in the induction regimen. Switch maintenance can be understood as an early second-line therapy. Differences in efficacy between these two maintenance strategies remain unknown. A recent meta-analysis did not detect any significant differences in OS or progression-free survival (PFS) between these two maintenance strategies.8 In contrast, another two meta-analyses showed favorable OS benefits for switch maintenance.9,10 In the study by Behera et al, switch maintenance provided significant benefit, both in PFS (hazard ratio [HR] 0.62, 95% confidence interval [CI] 0.57–0.67, P<0.0001) and OS (HR 0.84, 95% CI 0.77–0.91, P=0.00026). In contrast, continuation maintenance modestly improved PFS (HR 0.90, 95% CI 0.85–0.95, P=0.007), but did not show an OS benefit (HR 0.927, 95% CI 0.78–1.09, P=0.33).9 In the study by Cai et al, PFS was prolonged by both continuation (HR 0.54, 95% CI 0.46–0.63, P<0.00001) and switch (HR 0.64, 95% CI 0.59–0.70, P<0.00001) maintenance. Switch maintenance significantly improved OS (HR 0.80, 95% CI 0.72–0.90, P=0.0002), while continuation maintenance did not achieve a statistically significant improvement (HR 0.82, 95% CI 0.66–1.01, P=0.06).10 From the viewpoint of clinical practice, these two maintenance strategies are very different, especially at the time of transition from the induction phase to the maintenance phase. Most oncologists would hesitate to discontinue an effective and tolerable induction regimen and then introduce a new drug with unknown efficacy and adverse effects. Thus, continuation maintenance is more acceptable than switch maintenance.
Currently, there are three drugs, comprising two molecular targeted drugs and one cytotoxic drug, approved as maintenance monotherapy after platinum-based induction chemotherapy: erlotinib (Tarceva®, Hoffmann-La Roche Ltd, Basel, Switzerland), a reversible epidermal growth factor receptor (EGFR) tyrosine kinase inhibitor (TKI), as switch maintenance for patients with any NSCLC histology; bevacizumab (Avastin®, Hoffmann-La Roche Ltd), a humanized monoclonal antibody that inhibits vascular endothelial growth factor and thereby angiogenesis, as continuation maintenance after platinum-based and bevacizumab-containing triplet induction for patients with non-squamous NSCLC; and pemetrexed as both types of maintenance for patients with non-squamous NSCLC.
Efficacy, safety, and tolerability of pemetrexed maintenance therapy
Pemetrexed is the only successful cytotoxic drug in maintenance therapy. There are three cytotoxic drugs that have been tested as candidates of continuation maintenance in phase III trials, but they showed different results (Table 4). Paclitaxel improved neither PFS nor OS,11 gemcitabine prolonged only PFS but not OS,12–14 and only pemetrexed successfully extended both PFS and OS.15,16 In addition, severe adverse effects were less frequent during the pemetrexed maintenance phase, compared indirectly with paclitaxel and gemcitabine maintenance (Table 5). Thus, pemetrexed had an advantage of less cumulative toxicity and better tolerability.
Table 4.
Phase III studies comparing a maintenance cytotoxic monotherapy with observation alone after induction chemotherapy
| Reference | PEP | n | Induction | Maintenance | PFS or TTP (M) | HR P-value |
OS (M) | HR P-value |
|---|---|---|---|---|---|---|---|---|
| Continuation maintenance | ||||||||
| Belani et al11 | RR | 401 enrolled | 3 regimens of CBDCA + PTX (arm 1–3)a | |||||
| TTP | 130 randomized | Survival from randomization before induction chemotherapy | ||||||
| 65 | w PTX | 8.9 | P=0.124 | 17.5 | P=0.243 | |||
| 65 | Obs | 6.8 | 14.0 | |||||
| Brodowicz et al13 (CECOG trial) | TTP | 352 induction | CDDP + GEM ×4 cycles | |||||
| 257 non-PD | ||||||||
| 215 randomized | Survival from first treatment administration | |||||||
| 138 | GEM | 6.6 | HR ND | 13.0 | HR ND | |||
| 68 | Obs | 5.0 | P<0.001 | 11.0 | P=0.195 | |||
| Survival from randomization after induction chemotherapy | ||||||||
| 138 | GEM | 3.6 | HR ND | 10.2 | HR ND | |||
| 68 | Obs | 2.0 | P<0.001 | 8.1 | P=0.172 | |||
| Belani et al12 | OS | 519 enrolled | CBDCA + GEM ×4 cycles | |||||
| 255 randomized | Probably from randomization after induction chemotherapy | |||||||
| 128 | GEM | 3.9 | HR ND | 8.0 | HR 0.97 | |||
| 127 | Obs | 3.8 | P-value ND | 9.3 | P=0.84 | |||
| Perol et al14 (IFCT-GFPC0502 trial) | PFS | 834 enrolled | CDDP + GEM ×4 cycles | |||||
| 464 randomized | Survival from randomization after induction chemotherapy | |||||||
| 154 | GEM | 3.8 | HR 0.56 | 12.1 | HR 0.89 | |||
| 155 | Obs | 1.9 | P<0.001 | 10.8 | P=0.3867 | |||
| Paz-Ares et al15,16 (PARAMOUNT trial) | PFS | 939 induction | CDDP + PEM ×4 cycles | OS of randomly assigned patients, from start of induction | ||||
| 539 non-PD | chemotherapy | |||||||
| 359 | PEM | 16.9 | HR 0.79 | |||||
| 180 | Obs | 14.0 | P=0.0191 | |||||
| Survival from randomization after induction chemotherapy | ||||||||
| 359 | PEM | 4.4 | HR 0.60 | 13.9 | HR 0.78 | |||
| 180 | Obs | 2.8 | P<0.001 | 11.0 | P=0.0198 | |||
| Switch maintenance | ||||||||
| Ciuleanu et al29 (JMEN trial) | PFS | Plt-based regimens ×4 cycles | Survival from randomization after induction chemotherapy | |||||
| 441 | PEM | 4.3 | HR 0.50 | 13.4 | HR 0.79 | |||
| 222 | Placebo | 2.6 | P<0.0001 | 10.6 | P=0.012 | |||
Notes:
Arm 1, CBDCA (AUC 6 mg/mL ⋅ min, day 1) plus PTX (100 mg/m2, days 1, 8, and 15) every 4 weeks; arm 2, CBDCA (AUC 2 mg/mL min, days 1, 8, and 15) plus PTX (100 mg/m2, days 1, 8, and 15) every 4 weeks; arm 3, CBDCA (AUC 2 mg/mL ⋅ min) plus PTX (150 mg/m2 in cycle 1 and 100 mg/m2 in cycle 2) weekly for 6 of 8 weeks.
Abbreviations: AUC, area under the curve; CDDP, cisplatin; GEM, gemcitabine; HR, hazard ratio; M, months; ND, not described; Obs, observation alone; OS, overall survival; PEP, primary endpoint; PD, progressive disease; PEM, pemetrexed; PFS, progression-free-survival; Plt, platinum; PTX, paclitaxel; RR, overall response rate; TTP, time to progressive disease; w PTX, weekly paclitaxel.
Table 5.
Comparison of grade 3–4 adverse events during monotherapy maintenance phase (incidence rate ≥1% in any study)
| Reference
|
Brodowicz et al13 (CECOG trial)
|
Belani et al12
|
Perol et al14 (IFCT-GFPC0502 trial)
|
Paz-Ares et al16 (PARAMOUNT trial)
|
Ciuleanu et al29 (JMEN trial)
|
||||
|---|---|---|---|---|---|---|---|---|---|
| n | 138 | 128 | 127 | 154 | 155 | 359 | 180 | 441 | 222 |
| Maintenance regimens | GEM | GEM | BSC | GEM | BSC | PEM | BSC | PEM | BSC |
| Hematologic | |||||||||
| Leukopenia (%) | 2.3 | ND | ND | ND | ND | 2.2 | 0 | 2 | <1 |
| Neutropenia (%) | 14.9 | 13.3 | 1.6 | 20.8 | 0.6 | 5.8 | 0 | 3 | 0 |
| Anemia (%) | 2.6 | 9.4 | 2.4 | 2.6 | 0.6 | 6.4 | 0.6 | 3 | <1 |
| Thrombocytopenia (%) | 1.7 | 9.4 | 1.4 | 6.5 | 0 | 1.9 | 0 | ND | ND |
| Non-hematologic | |||||||||
| Fatigue (%) | ND | 3.9 | 1.6 | ND | ND | 4.7 | 1.1 | 5 | <1 |
| Alopecia (%) | 4.3 | ND | ND | ND | ND | ND | ND | ND | ND |
| Deterioration of general condition (%) | ND | ND | ND | 3.2 | 3.9 | ND | ND | ND | ND |
| Pneumonia (%) | ND | ND | ND | 3.2 | 1.3 | ND | ND | ND | ND |
| Anorexia (%) | ND | ND | ND | 0.6 | 0.6 | 0.3 | 0 | 2 | 0 |
| Asthenia (%) | ND | ND | ND | 1.9 | 0 | ND | ND | ND | ND |
| Febrile neutropenia (%) | ND | ND | ND | ND | ND | 1.9 | 0 | ND | ND |
| Infection (%) | ND | ND | ND | 1.3 | 0 | ND | ND | 2 | 0 |
| Pain (%) | ND | ND | ND | ND | ND | 1.1 | 0 | ND | ND |
Notes: Study by Brodowicz et al (CECOG trials)13 did not describe adverse events in the control arm. No study compared adverse events statistically.
Abbreviations: BSC, best supportive care; GEM, gemcitabine; ND, not described; PEM, pemetrexed.
Erlotinib switch maintenance has never been compared with pemetrexed switch or continuation maintenance in a head-to-head Phase III trial. Bevacizumab combined with carboplatin plus paclitaxel has been directly compared with pemetrexed continuation maintenance in two Phase III studies (Table 6).17,18 These two studies, PRONOUNCE and ERACLE, defined unique primary endpoints of PFS without grade 4 adverse events18 and difference in QoL,17 respectively, instead of the usual efficacy parameters of PFS or OS. Thus, these studies provided little information with regard to deciding which regimen is superior as the first-line regimen for patients with non-squamous NSCLC.
Table 6.
Phase III studies comparing bevacizumab with pemetrexed or pemetrexed plus bevacizumab
| Reference | PEP | n | Induction | Maintenance | PFS (M) |
HR P-value |
OS (M) |
HR P-value |
|---|---|---|---|---|---|---|---|---|
| Zinner et al18 (PRONOUNCE trial) | G4PFS | 361 | CBDCA + PEM | PEM | Survival from random assignment before induction chemotherapy G4PFS | |||
| CBDCA + PTX + Bev ×6 cycles | Bev | |||||||
| 182 | PEM | 3.9 | HR 0.85 | 10.5 | HR 1.07 | |||
| 179 | Bev | 2.9 | P=0.176 | 11.7 | P=0.615 | |||
| PFS | ||||||||
| 182 | PEM | 4.4 | HR 1.06 | |||||
| 179 | Bev | 5.5 | P=0.61 | |||||
| Galetta et al17 (ERACLE trial) | QoLa | 118 | ||||||
| 60 | CDDP + PEM | PEM | ND | HR 0.62 | ND | HR 0.69 | ||
| 58 | CBDCA + PTX + Bev ×6 cycles | Bev | ND | P=0.03 | ND | P=0.08 | ||
| Barlesi et al34,35 (AVAPERL trial) | PFS | 376 induction | CDDP + PEM + Bev ×4 cycles | |||||
| 253 non-PD | Survival from random assignment after induction chemotherapy | |||||||
| 128 | PEM + Bev | 7.4 | HR 0.57 | 17.1 | HR 0.87 | |||
| 125 | Bev | 3.7 | P<0.0001 | 13.2 | P=0.29 | |||
| Patel et al36 (PointBreak trial) | OS | |||||||
| 934 randomized | Survival from random assignment before induction treatment | |||||||
| 472 | CBDCA + PEM + Bev | PEM + Bev | 6.0 | HR 0.83 | 12.6 | HR 1.00 | ||
| 467 | CBDCA + PTX + Bev ×4 cycles | Bev | 5.6 | P=0.012 | 13.4 | P=0.949 | ||
Note:
EQ5D Index (EQ5D-I) and EQ5D-VAS (Euro-QoL questionnaire) at 12 weeks during maintenance therapy.
Abbreviations: Bev, bevacizumab; CBDCA, carboplatin; CDDP, cisplatin; G4PFS, progression-free survival without grade 4 adverse event; HR, hazard ratio; M, months; ND, not described; OS, overall survival; PD, progressive disease; PEM, pemetrexed; PEP, primary endpoint; PFS, progression-free survival; PTX, paclitaxel; QoL, quality of life.
Cost-effectiveness of pemetrexed maintenance therapy
The cost-effectiveness of maintenance treatment with pemetrexed monotherapy is debatable (Table 7). There were five pharmacoeconomic analyses from various countries addressing this problem.19–23 Four analyses were based on a switch maintenance trial (JMEN),19–22 while the other was a continuation maintenance trial (PARAMOUNT).23 Three of these analyses concluded that pemetrexed maintenance is not cost-effective, irrespective of switch and continuation.21–23 In the pharmacoeconomic analyses from Japan, Switzerland, and the People’s Republic of China, each willingness-to-pay threshold was assumed as ¥5–6 million per LYG (US $43,478–52,174 per LYG),22 €72,000 per QALY gained (Swiss federal court decision, November 23, 2010),21 and US $13,527 per QALY gained (3× the per capita gross domestic product),23 respectively. All ICERs based on LYG or QALY were more than these thresholds.21–23 The UK analysis also found that the most plausible ICER was £47,000 per QALY gained, which was above the standard NICE willingness-to-pay range (£20,000 to £30,000 per QALY).19 Considering that maintenance treatment with pemetrexed fulfilled the end-of-life criteria, NICE in the UK optionally recommended switch maintenance by pemetrexed only for patients with non-squamous histology.24 In contrast, NICE did not recommend continuation maintenance by pemetrexed because the most plausible ICER, approximately £74,500 per QALY gained, was higher than that normally considered to be cost-effective, even if the supplementary advice of NICE on end-of-life treatments was taken into consideration.25 The US analysis indicated that pemetrexed may be considered cost-effective.20 The ICER for pemetrexed to observation alone, ie, US $122,371, may not be cost-effective when compared with a commonly mentioned threshold of US $100,000 per LYG, but may be cost-effective when compared with a range of US $95,000 to US $264,000 per LYG, a recently revised plausible lower and upper bounds for cost-effectiveness decision rule in the USA.26
Table 7.
Comparison in cost-effectiveness of direct medical cost between maintenance with pemetrexed vs. observation alone after induction chemotherapy: study designs and results
| Reference | Methods, costs and outcomes discount, study perspective, time frame and reference year for cost | Data sources | Study population | Regime | Cost | LYG or OS | QALY | ICERa/LYG | ICERa/QALY |
|---|---|---|---|---|---|---|---|---|---|
| Greenhalgh et al19 (UK) | ERG report reviewing the manufacturer’s evidence submission, de novo economic model Cost discount ND Time frame; lifetime Reference year; ND |
Clinical parameters: RCT (JMEN trial) | Subgroup of 481 patients in JMEN trial | PEM maintenance | 15.5 M | ||||
| Submitted base caseb | £17,455 | 0.9697 | ND | £33,732 | |||||
| Combined effect of changes | £20,925 | 0.9539 | ND | £47,239 | |||||
| BSC alone | 10.3 M | ||||||||
| Submitted base caseb | £8,318 | 0.6988 | |||||||
| Combined effect of changes | £8,370 | 0.6881 | |||||||
| Klein et al20 (US) | Semi-Markov model Discounted at 3% US payer’s perspective Time frame; 3 years Reference; 2009 US$ |
Clinical parameters: RCT (JMEN, ATLAS, SATURN trials) Cost: Medicare reimbursement rate and analysis of claim database (PharMetrics) |
Advanced NSCLC patients who have completed first-line platinum double chemotherapy without progression | PEM maintenance | |||||
| Non-SQ | $96,774 | 1.3412 Y | $122,371 | ||||||
| All NSCLC | $89,289 | 1.2434 Y | $205,597 | ||||||
| BSC alone | ND | ND | |||||||
| Non-SQ | $64,830 | 1.0802 Y | |||||||
| All NSCLC | $61,036 | 1.1060 Y | |||||||
| Tsuchiya et al22 (Japan) | Markov model Discounted at 3% annually Japanese healthcare payer perspective Time frame; ND Reference; 2009 US$ (assumed US $1 to JPY 115) |
Clinical parameters: RCT (JMEN trial) | Advanced NSCLC (either non-SQ or all histology), Japanese men in their 60s, height 164.6 cm, weight 64.5 kg, BSA 1.70 m2 | PEM maintenance | |||||
| Non-SQ | $68,536 | 489.4 D | 0.7321 | $80,563 | $150,115 | ||||
| All NSCLC | $64,409 | 451.8 D | 0.6770 | $109,024 | $203,022 | ||||
| BSC alone | |||||||||
| Non-SQ | $39,872 | 359.5 D | 0.5411 | ||||||
| All NSCLC | $38,843 | 366.2 D | 0.5511 | ||||||
| Matter-Walstra et al21 (Switzerland) | Markov model No discount Swiss health care system perspective Time frame; lifetime Reference; 2010 Swiss prices (€0.72 / Swiss franc) |
Clinical parameters: RCT (JMEN trial) Cost: literature | Advanced non-SQ NSCLC, BSA 1.77 m2 |
PEM maintenance | €99,705 | 15.6 M | 0.82 | ND | €106,202 |
| BSC alone | €71,316 | 10.7 M | 0.56 | ||||||
| Zeng et al23 (People’ Republic of China) | Markov model Discounted at 3% annually Chinese health care system perspective Time frame; 1,2,5 and 10 year Reference; 2010 US$ (assumed 1 US$ to 6.6515 Chinese yuan) |
Clinical parameters: RCT (PARAMOUNT trial) Cost: BSC and AE costs from literature, market share and local charges in the People’s Republic of China |
Advanced non-SQ NSCLC, weight 65 kg, BSA 1.72 m2 |
PEM maintenance | |||||
| 1-year | $36,443 | 0.760 Y | 0.440 | $193,796 | $183,589 | ||||
| 2-year | $55,532 | 1.140 Y | 0.631 | $99,183 | $126,353 | ||||
| 5-year | $72,103 | 1.444 Y | 0.776 | $80,792 | $124,766 | ||||
| 10-year | $73,955 | 1.477 Y | 0.791 | $79,134 | $124,793 | ||||
| BSC alone | |||||||||
| 1-year | $28,255 | 0.718 Y | 0.396 | ||||||
| 2-year | $44,181 | 1.026 Y | 0.541 | ||||||
| 5-year | $54,790 | 1.230 Y | 0.637 | ||||||
| 10-year | $55,607 | 1.245 Y | 0.644 |
Notes:
Incremental pemetrexed maintenance to BSC;
data based upon the evidence submission from the manufacturer (Eli Lilly) to the National Institute for Health and Clinical Excellence (NICE) as part of the single technology appraisal process.
Abbreviations: AE, adverse events; BSA, body surface area; BSC, best supportive care; D, days; ERG, evidence review group; ICER, incremental cost-effectiveness ratio; JPY, Japanese Yen; LYG, life-year gained; M, months; ND, not described; NSCLC, non-small cell lung cancer; OS, overall survival; PEM, pemetrexed; QALY, quality-adjusted life-year; RCT, randomized controlled trial; SQ, squamous cell carcinoma; Y, years.
Comparison of cost-effectiveness between different types of maintenance is more difficult because of a lack of head-to-head clinical trials. Three studies have indirectly compared direct medical costs between maintenance with pemetrexed and maintenance with another drug (Table 8).20,27,28 A US study showed that pemetrexed maintenance is more cost-effective for patients with non-squamous NSCLC than erlotinib, because the ICER for pemetrexed versus erlotinib (US $150,260/LYG) is within the acceptable range of willingness to pay.20 Another UK study also showed a clear advantage in favor of pemetrexed, ICER for erlotinib versus pemetrexed, £84,029/QALY gained.27 In contrast, a European cross-market cost comparison showed that total monthly treatment costs per patient, including acquisition costs, administration costs, and costs of treating adverse events, were more reasonable for erlotinib than for pemetrexed, ie, €2,140 for erlotinib versus €3,453 for pemetrexed in France, €2,732 versus €5,534 in Germany, €1,518 versus €2,921 in Italy, and €2,048 versus €3,164 in Spain.28 Thus, it remains unknown which maintenance strategy is the most cost-effective.
Table 8.
Comparison in cost-effectiveness of direct medical cost between pemetrexed and other maintenance therapy: study designs and results
| Reference | Methods, costs and outcomes discount, study perspective, time frame and reference year for cost | Data sources | Study population | Regime | Costs | LYG / OS | QALY | ICER / LYG | ICER / QALY |
|---|---|---|---|---|---|---|---|---|---|
| Klein et al20 (US) |
See Klein et al20 | PEM | |||||||
| Non-SQ | $96,774 | 1.3412 Y | ND | ||||||
| All NSCLC | $89,289 | 1.2434 Y | ND | ||||||
| Erlotinib | |||||||||
| Incremental PEM to Erlotinib | |||||||||
| Non-SQ | $72,300 | 1.1784 Y | ND | $ 150,260 | ND | ||||
| All NSCLC | $71,147 | 1.1854 Y | ND | $ 312,341 | ND | ||||
| Bev (15 mg/kg) | |||||||||
| Incremental Bev to PEM | |||||||||
| Non-SQ | $105,961 | 1.2933 Y | ND | Dominated | ND | ||||
| Dickson et al27 (UK) |
ERG report reviewing the manufacturer’s evidence submission, de novo economic model Cost discount; ND Time frame; lifetime Reference year; ND |
Clinical parameters: RCT (SATURN, JMEN trial) | Model 1; SD, All NSCLC: Erl vs. placebo Model 2; SD, SQ: Erl vs. placebo Model 3; SD, non-SQ: Erl vs. PEM |
PEM | |||||
| SD, non-SQ | £26,608 | 1.5495 Y | 0.9229 | ND | ND | ||||
| Erlotinib | |||||||||
| Incremental PEM to Erlotinib | |||||||||
| SD, non-SQ | £18,148 | 1.4213 Y | 0.8222 | ND | £84,029 | ||||
| Nuijten et al28 (France, Germany, Italy and Spain) |
Cross-market cost comparison Perspective of national health-care decision-makers or purchasers. Time frame; monthly Reference; 2008 Euro |
Clinical parameters: RCT (SATURN, JMEN trial) Cost; literatures, National drug tariffs for France, Germany, Italy and Spain |
Advanced NSCLC | PEM | ND | ND | ND | ND | |
| France | €3,453 | ||||||||
| Germany | €5,534 | ||||||||
| Italy | €2,921 | ||||||||
| Spain | €3,164 | ||||||||
| Erlotinib | ND | ND | ND | ND | |||||
| France | €2,140 | ||||||||
| Germany | €2,732 | ||||||||
| Italy | €1,518 | ||||||||
| Spain | €2,048 | ||||||||
Abbreviations: Bev, bevacizumab; Erl, erlotinib; ERG, Evidence Review Group; ICER, incremental cost-effectiveness ratio; LYG, life-year gained; ND, not described; NSCLC, non-small-ell lung cancer; OS, overall survival; PEM, pemetrexed; QALY, quality-adjusted life-year; RCT; randomized controlled trial; SD, stable disease; SQ, squamous cell carcinoma; Y, years.
There were many study limitations in these pharmacoeconomic analyses; for example, a lack of clinical trials and detailed information about quality of life, imbalanced accrual in trials, and a variety of medical services among countries and territories. A Japanese study of direct medical cost by Tsuchiya et al22 was based on clinical results of JMEN study29 and Japanese health care system. Although the JMEN study included 32% of Asian population in pemetrexed switch maintenance group mainly from the People’s Republic of China and Korea, no Japanese patient participated in this trial. The PARAMOUNT trial, undertaken in 93 center in 16 countries, included Asian population in only 4% of all cases.30 Therefore, we Japanese and Asian can not refer to clinical results of this trial for a pharmacoeconomic study. There were three Japanese single-arm, Phase II studies evaluating a combination of carboplatin plus pemetrexed followed by pemetrexed maintenance for patients with non-squamous NSCLC. These trials provided an impressive median OS of more than 20 months not only from maintenance chemotherapy in patients who had received maintenance therapy31,32 but also from induction chemotherapy in all enrolled patients.32,33 In contrast, the JMEN and PARAMOUNT studies showed a median OS of 16.5 and 16.9 months, respectively, from induction chemotherapy for patients who had proceeded into the maintenance phase (Table 9).15,16,29 OS in the Japanese single-arm, Phase II studies was much longer (by approximately 4 months) than in the multinational randomized placebo-controlled studies. Thus, the Japanese medical economic study possibly underestimated pemetrexed maintenance when based on clinical data from other ethnic groups and countries. Further studies and discussions are warranted with regard to pemetrexed maintenance.
Table 9.
Comparison of efficacy of the first-line combination of pemetrexed plus platinum followed by pemetrexed maintenance between Japanese Phase II studies and multinational Phase III studies
| Reference | Country | Phase | Patients | Treatment | PFS and OS from induction (M) |
|---|---|---|---|---|---|
| Ciuleanu et al29 (JMEN trial) |
Multi | R-p3 | 441 NSCLC, including 26% SQ | Plt-based doublet ×4 cycles | PFS 7.7 |
| → PEM maintenance | OS 16.5 | ||||
| Paz-Ares et al15,16 (PARAMOUNT trial) |
Multi | R-p3 | 359 non-SQ | CDDP + PEM ×4 cycles | PFS ND |
| → PEM maintenance | OS 16.9 | ||||
| Okamoto et al33 (JACAL trial) |
Japan | S-p2 | 109 non-SQ | CBDCA + PEM ×4 cycles | PFS 5.7 |
| → PEM maintenance | OS 20.2 | ||||
| Minami et al32 (OULCSG0902 trial) |
Japan | S-p2 | 34 non-SQ | CBDCA + PEM ×4 cycles | PFS 5.2 |
| → PEM maintenance | OS 23.3 | ||||
| Karayama et al31 | Japan | R-p2 | 26 non-SQ | CBDCA + PEM ×4 cycles | PFS 7.4 |
| → PEM maintenance | OS 25.0 |
Abbreviations: CBDCA, carboplatin; CDDP, cisplatin; M, month; Multi, multinational; ND, not described; NSCLC, non-small-cell lung cancer; OS, overall survival; PEM, pemetrexed; PFS, progression-free survival; Plt, platinum; R-p2, randomized phase II; R-p3, randomized phase III; S-p2, single-arm phase II; SQ, squamous cell carcinoma.
Future directions
A recent interesting challenge is doublet combination maintenance (Table 6).34–36 We may have to consider EGFR mutation status for selection of a combination pattern. For patients with non-squamous NSCLC histology and positive EGFR mutation status, combination patterns of EGFR TKI with pemetrexed or bevacizumab are promising. A randomized Phase III trial is underway comparing gefitinib monotherapy with doublet continuation maintenance of pemetrexed plus gefitinib after triplet induction with carboplatin, pemetrexed, and gefitinib in patients with non-squamous NSCLC and positive EGFR mutations (NEJ009, trial number: UMIN000006340). This study potentially develops a first-line regimen for such patients. On the other hand, combination maintenance of bevacizumab plus an EGFR TKI is an alternative candidate treatment for these patients. Erlotinib provided an add-on effect with regard to PFS (bevacizumab plus placebo versus bevacizumab plus erlotinib; 3.7 versus 4.8 months from time of random assignment after induction chemotherapy, HR 0.71, 95% CI 0.58–0.86, P<0.001), but failed in OS (13.3 versus 14.4 months, respectively, HR 0.92, 95% CI 0.70–1.21, P=0.5341), when a maintenance combination of erlotinib plus bevacizumab was introduced after four cycles of a bevacizumab-containing platinum-doublet chemotherapy for NSCLC patients who had not been selected by EGFR mutation status (ATLAS).37 For a subgroup with active EGFR mutations, compared with the wild-type subgroup, this combination maintenance therapy also achieved greater improvement in PFS (HR 0.44, 95% CI 0.22–0.86 for the EGFR mutation-positive subgroup [n=52] versus HR 0.85, 95% CI 0.64–1.13 for the EGFR wild-type subgroup [n=295]), but there was no statistically significant difference in OS outcome (HR 0.46, 95% CI 0.21–1.02 versus HR 0.86, 95% CI 0.65–1.15, respectively). Thus, for patients with wild-type EGFR and unknown EGFR mutation status, maintenance therapy of bevacizumab plus erlotinib is not recommended, while subgroup analyses of this randomized Phase III study suggested a potential efficacy of this maintenance combination for patients with active EGFR mutations. A recent randomized Phase II study in Japan (JO25567) also demonstrated that first-line bevacizumab plus erlotinib markedly improved PFS compared with erlotinib alone (16.0 months for erlotinib plus bevacizumab [n=77] versus 9.7 months for erlotinib alone [n=77], HR 0.54, 95% CI 0.36–0.79, P=0.0015).38 This study suggests that, for patients with active EGFR mutation status, combination of these two molecularly targeted drugs potentially yields a better survival benefit than erlotinib alone. We hope that this combination is beneficial in the maintenance setting, as well as in the first-line setting.
For patients with non-squamous NSCLC and wild-type or unknown EGFR mutation status, pemetrexed plus bevacizumab is possibly promising. Compared with bevacizumab alone, continuation maintenance of pemetrexed plus bevacizumab significantly prolonged PFS by a median of 3.7 months, but did not achieve a significant improvement in OS, despite a difference of 3.9 months in median OS after four cycles of bevacizumab combined with cisplatin plus pemetrexed (AVAPERL).35 Another Phase III study (PointBreak) showed that continuation maintenance of pemetrexed plus bevacizumab after an induction triplet of bevacizumab combined with carboplatin plus pemetrexed was similar in OS but significantly superior in PFS when compared with continuation maintenance of bevacizumab alone after bevacizumab combined with carboplatin plus paclitaxel.36 Thus, even the combination of pemetrexed plus bevacizumab remains unable to show an OS benefit when compared with bevacizumab alone. Adverse effects of anemia, thrombocytopenia, and fatigue were significantly more frequent on combination maintenance than on bevacizumab alone in the PointBreak trial (Table 10).36 Benefit in terms of cost-effectiveness should be investigated for these combination maintenance therapies when their significant survival benefits are demonstrated, because these drugs are all very expensive.
Table 10.
Comparison of grade 3–4 adverse events during maintenance phase (incidence rate ≥1% in any study)
| Reference
|
Barlesi et al34,35 (AVAPERL trial)
|
Patel et al36 (PointBreak trial)
|
||
|---|---|---|---|---|
| n | 125 | 120 | 292 | 298 |
| Maintenance regimen | PEM + Bev | Bev | PEM + Bev | Bev |
| Hematologic | ||||
| Leukopenia (%) | ND | ND | ND | ND |
| Neutropenia (%) | 5.6 | 0 | 14.0 | 11.4 |
| Anemia (%) | 3.2 | 0 | 11.0a | 0.3 |
| Thrombocytopenia (%) | 0 | 0 | 7.2a | 2.3 |
| Non-hematologic | ||||
| Fatigue (%) | 2.4 | 1.7 | 9.6a | 1.7 |
| Hypertension (%) | 4.8 | 2.5 | 3.1 | 6.0 |
| Sensory neuropathy (%) | ND | ND | 0a | 4.7 |
| Thromboembolic events (%) | ND | ND | 2.4 | 0.7 |
| Pulmonary embolism (%) | 0.8 | 1.7 | ND | ND |
| GI or pulmonary hemorrhage (%) | ND | ND | 1.4 | 0 |
| Febrile neutropenia (%) | 0.8 | 0 | 1.0 | 0 |
Notes: AVAPERL study did not describe the result of statistical comparison.
Statistically significant (P<0.05).
Abbreviations: Bev, bevacizumab; GI, gastrointestinal; ND, not described; PEM, pemetrexed.
For the future, we may need to narrow the core patients who are predicted to benefit from maintenance therapy with pemetrexed or other drugs. Hence, more clear-cut markers are required, such as EGFR mutation status for NSCLC. The most promising predictive biomarker of the efficacy of pemetrexed at this time is the thymidylate synthase expression level. Basic research is warranted to identify a reliable biomarker than can predict the clinical benefit of pemetrexed. These personalized therapies represent appropriate treatment options and result in cost savings when using expensive drugs. Investigation of selection or exclusion biomarkers is warranted.
Footnotes
Disclosure
The authors report no conflicts of interest in this work.
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