DOI: https://doi.org/10.21203/rs.3.rs-72198/v1
Background
Irinotecan (IRI) and oxaliplatin (Ox) are standard therapeutic agents of the first-line treatments for metastatic colorectal cancer (mCRC). Previous meta-analyses of randomized controlled trials (RCTs) showed that treatment with Ox-based compared with IRI-based regimens was associated with better overall survival (OS). However, these reports did not include trials of molecular targeting agents and did not take methods for the administration of concomitant drugs, such as bolus or continuous infusion of 5-fluorouracil, into account. A systematic literature review was performed to compare the efficacy and toxicity profiles between IRI- and Ox-based regimens as the first-line treatments for mCRC.
Methods
This meta-analysis used data from the Cochrane Central Register of Controlled Trials, PubMed, and SCOPUS. The primary endpoint was OS, and the secondary endpoints were progression-free survival (PFS), objective response rate (ORR), and adverse events (AEs).
Results
Nineteen trials involving 4,571 patients were included in the analysis. No statistically significant difference was observed between the two groups in terms of OS, PFS, and ORR. There was no significant heterogeneity. Regarding ≥ grade 3 AEs, IRI-based regimens were associated with a high incidence of leukopenia, febrile neutropenia, and diarrhea. Moreover, there was a high incidence of thrombocytopenia and peripheral sensory neuropathy in patients who received Ox-based regimens. In a subgroup analysis, IRI combined with bevacizumab was correlated with a better PFS (HR = 0.90, 95% CI = 0.82–0.98, P = 0.02), but not with OS.
Conclusion
Although the safety profiles of IRI- and Ox-based regimens varied, their efficacy did not significantly differ. Therefore, both regimens could be used as the first-line treatments for mCRC with consideration of the patients’ condition or toxicity profiles.
Currently, colorectal cancer (CRC) ranks fourth for incidence worldwide, with 550,000 deaths recorded annually.1 Patients with unresectable metastatic CRC (mCRC) have a poor prognosis, with a median overall survival (OS) of 6–8 months, without any therapy. Although chemotherapy is the standard treatment for these patients, the median OS is only 20–25 months.2
The combination of cytotoxic and molecular targeting agents is currently used as the first-line treatment for patients with unresectable mCRC. Irinotecan (IRI) or oxaliplatin (Ox) combined with fluoropyrimidines (FPs) is considered as the backbone of cytotoxic agents for the treatment of mCRC.3 In the meta-analysis conducted by Grothey et al.4, the use of all three active drugs (FPs, IRI, and Ox) for mCRC was associated with a long OS.
First-line treatment is important for patients with mCRC, because the treatment period is the longest of the overall treatment time and significantly affects survival and quality of life (QOL). With regard to the use of cytotoxic agents, several trials investigated the best combination of regimens. Tournigand et al.5 and Colucci et al.6 conducted clinical trials to compare the efficacy between 5-fluorouracil (5-FU), folinic acid, and Ox (FOLFOX) regimen and 5-FU, folinic acid, and IRI (FOLFIRI) regimen. Results showed no significant differences between the two regimens. Moreover, Yamazaki et al.7 compared these regimens with bevacizumab (BEV), a molecular targeting agent. Results showed that the OS did not significantly differ between patients who received FOLFOX + BEV and FOLFIRI + BEV. Hence, both IRI- and Ox-based regimens could be used as the first-line treatments for mCRC.
In clinical practice, physicians generally select the regimen based on adverse events (AEs) caused by the drugs or the patients’ condition. Recent reports showed that physicians preferred Ox-based regimen than IRI-based regimen. Field et al.8 conducted a survey on the use of chemotherapy for CRC. Results showed that 92.6% of medical oncologists in Australia select Ox-based regimen as the first-line treatment. They reported physicians commonly select this regimen as it has better efficacy and lower toxicity than IRI-based regimen. In addition, Marschner et al.9 conducted a prospective cohort study and revealed that Ox-based regimen was used as the first-line treatment in 430 out of 605 patients (71.0%) with mCRC.
Previous meta-analyses10–12 of the first-line treatments for mCRC revealed that Ox-based regimen was correlated with a better OS. However, these studies included trials comparing continuous 5-FU infusion regimen with bolus 5-FU regimen, which is currently considered an inferior method. Moreover, these data were obtained from reports of regimens without molecular targeting agents. Therefore, they might not be applicable in the current clinical practice. Recently, a population-based observational study conducted by Teng et al.13 reported that IRI-based regimen might be more effective in improving OS than Ox-based regimen. Therefore, it remains unclear which regimen is associated with a better OS. Thus, a meta-analysis based on the current knowledge was performed to compare the efficacy and toxicity between IRI- and Ox-based regimens as the first-line treatments for mCRC.
We searched PubMed, SCOPUS, and the Central Registry of Controlled Trials of the Cochrane Library (CENTRAL) without language restrictions. The last search update was performed on December 17, 2018. The inclusion criteria were as follows: (1) randomized controlled trials comparing IRI- and Ox-based combination regimens as the first-line treatments for mCRC and (2) those using similar agents (IRI- or Ox-based combination regimens) or agents with comparable efficacy based on the results of previous randomized controlled trials. The efficacy of oral FPs was similar to that of continuous infusion of 5-FU. That is, capecitabine + Ox (CapOx) regimen and S-1 + Ox (SOX) regimen were considered as alternative to FOLFOX regimen.14–16 Similarly, capecitabine + IRI (CapIRI) and S-1 + IRI (IRIS) regimens were considered as alternative to FOLFIRI regimen.17, 18 (3) Abstracts or unpublished data were included if they had sufficient information on study design, characteristics of participants, interventions, and outcomes.
The search terms used were as follows: (1) terms suggestive of “colorectal” (i.e., “colorect*,” “colon,” “colonic,” “bowel*,” “recta*,” or “rectum”), (2) “cancer” (i.e., “cancer,” “carcinoma*,” “neoplas*,” or “tumor”), (3) “irinotecan” (i.e., “irinotecan,” “camptotecin-11,” or “topotecin”), (4) “oxaliplatin” (i.e., “L-OHP,” “eloxatine,” or “oxaliplatin”), and (5) “randomized trials” (i.e., “ramdomized controlled,”,“randomised,” or “randomly”).
At least two of three review authors (SK, NT, and YH) independently scanned titles and abstracts to exclude studies that do not meet the criteria. The full text reports were then reviewed for further assessment. Disagreements were resolved via a consensus. Detailed data from eligible trials, such as year of publication, place where the study was conducted, study design, regimens, participants’ information, methodological evaluation, outcomes, and AEs, were extracted. If necessary, the authors were contacted for clarifications.
At least two of three authors (SK, NT, and YH) independently assessed the risk of bias in the included studies in accordance with the Cochrane Handbook for Systematic Reviews of Interventions.19 The following domains were assessed: (1) sequence generation; (2) allocation concealment; (3) blinding of participants, personnel, and outcome assessors; (4) incomplete outcome data; (5) selective outcome reporting; and (6) other potential threats to validity. When inadequate details of methodological characteristics of trials were provided, the authors were contacted to obtain further information.
The primary endpoint was OS. The secondary endpoints were progression-free survival (PFS), objective response rate (ORR), and ≥ grade 3 AEs according to the Common Terminology Criteria for Adverse Events version 4.0. Hazard ratios (HRs) and 95% confidence interval (CI), which were considered as relevant effect measures, were directly or indirectly assessed using the given data. When the Kaplan–Meier curve, but not the HR for PFS or OS, was included, we extracted the value using the Engauge Digitizer 10.8 and the method provided by Tierney et al.20 ORR were compared using odds ratio (OR). The risk difference was used to compare the risk of AEs. Statistical heterogeneity among the studies was assessed using the chi-square test and was expressed with the I2 index.19 The pooled effect was calculated with the random-effects model. Subgroup analyses were performed according to the combination of agents, which include regimens with or without molecular targeting agents, infusion of 5-FU or oral FPs, and anti-epidermal growth factor receptor (EGFR) or anti-ca (VEGF) antibodies. Since a previous report showed that CapOx plus anti-EGFR antibody might be less effective than FOLFOX plus anti-EGFR,21 we added the subgroup of anti-EGFR antibodies except CapOx + cetuximab. Statistical analyses were performed using the RevMan 5.3 software, which was provided by The Cochrane Collaboration. The corresponding funnel plots were used to examine the effect of publication bias visually. A two-sided P-value < 0.05 was considered statistically significant.
A total of 4,451 potentially relevant studies were retrieved from the initial database search in PubMed, SCOPUS, and CENTRAL. Of these studies, 22 met all the inclusion criteria. However, one trial did not provide sufficient data, 22 and two were discontinued early due to poor accrual.23, 24 Finally, 19 RCTs5–7, 25–40 with 4,571 patients were included in the analysis. A flowchart of the search process is shown in Fig. 1.
Table 1 shows the characteristics of RCTs included in the meta-analysis. Of these, 12 trials (n = 3,534) used 5-FU infusion regimens; 6 (n = 943), oral FPs; and 1, raltitrexed (n = 94). Nine RCTs (n = 2,154) used regimens with molecular targeting agents. Among them, five used BEV and four anti-EGFR antibodies (cetuximab or panitumumab). In total, 2 RCTs were conducted in North America, 13 in Europe, and 4 in Asia. The median age of the participants in all studies was 61–75 years. In one trial32, only elderly patient aged > 70 years was eligible.
Study no. |
Authors |
Region |
Year |
Trial phase |
Primary endpoint |
Interventions |
Patients |
Median OS (months) |
1 |
Grothey et al.25 |
USA |
2003 |
2 |
AEs |
CapOx |
82 |
NA |
2 |
Tournigand et al.5 |
France |
2004 |
3 |
PFS |
FOLFOX |
113 |
20.6 |
3 |
Kalofonos et al.26 |
Greece |
2005 |
2 |
ORR |
Weekly Ox + LV + 5-FU |
148 |
17.4 |
4 |
Comella et al.27 |
Italy |
2005 |
3 |
ORR |
OXAFAFU |
140 |
18.9 |
5 |
Colucci et al.6 |
Italy |
2005 |
3 |
ORR |
FOLFOX |
182 |
15 |
6 |
Feliu et al.28 |
Spain |
2005 |
2 |
ORR |
Raltitrexed + Ox |
48 |
NA |
7 |
Zheng et al.29 |
China |
2006 |
2 |
ORR |
FOLFOX7 |
30 |
NA |
8 |
Bajetta et al.30 |
Italy |
2007 |
2 |
AEs |
TEGAFOX |
73 |
19 |
9 |
Seymour et al.31 |
UK |
2007 |
3 |
OS |
OxFU |
357 |
15.4 |
10 |
Rosati et al.32 |
Italy |
2010 |
2 |
ORR |
CapOx |
47 |
19.3 |
11 |
Ocvirk et al.33 |
Germany |
2010 |
2 |
PFS |
FOLFOX6 + Cmab |
77 |
17.4 |
12 |
Moosmann et al.34 |
Germany |
2011 |
2 |
ORR |
CapOx + Cmab |
92 |
25.5 |
13 |
Schmiegel et al.35 |
Germany |
2013 |
2 |
PFS |
CapOx + BEV |
127 |
24.4 |
14 |
Folprecht et al.36 |
Germany |
2014 |
2 |
ORR |
FOLFOX6 + Cmab |
56 |
35.8 |
15 |
Yamazaki et al.7 |
Japan |
2016 |
3 |
PFS |
FOLFOX6 + BEV |
200 |
30.4 |
16 |
Parikh et al.37 |
USA |
2018 |
2 |
PFS |
FOLFOX6 + BEV |
188 |
23.9 |
17 |
Carrato et al.38 |
Spain |
2017 |
2 |
ORR |
FOLFOX4 + Pmab |
40 |
37 |
18 |
Yamada et al.39 |
Japan |
2018 |
3 |
PFS |
FOLFOX(CapOx) + BEV |
244 |
33.6 |
19 |
Nakayama et al.40 |
Japan |
2018 |
2 |
ORR |
CapOx + BEV |
54 |
26.7 |
OS, overall survival; AEs, adverse events; PFS, progression-free survival; ORR, objective response rate; NA, not available; CapOx, capecitabine + Ox; CapIRI, capecitabine + IRI; FOLFOX and OXAFAFU, 5-FU + folinic acid + Ox; FOLFIRI and IRIFAFU, 5-FU + folinic acid + IRI; TEGAFOX, tegafur + folinic acid + Ox; TEGAFIRI, tegafur + folinic acid + IRI; BEV, bevacizumab; Cmab, cetuximab; and Pmab, panitumumab |
Sixteen trials included data on OS (Fig. 2A). Since seven RCTs did not describe the HR for OS, we estimated the value using the Kaplan–Meier curve. Results showed no significant difference between IRI- and Ox-based regimens (pooled HR = 0.96, 95% CI = 0.89–1.03, P = 0.28), and there was no significant heterogeneity among the trials (I2 = 2%). Thirteen trials included data on PFS (Fig. 2B). We estimated the HR for PFS in six trials using the Kaplan–Meier curve. No significant difference was observed between the two groups (pooled HR = 0.98, 95% CI = 0.94–1.04, P = 0.49), and there was no significant heterogeneity (I2 = 0%). All trials included data on ORR (Fig. 2C). There was no significant difference between the two groups. However, Ox-based regimen had a favorable outcome (pooled OR = 1.13, 95% CI = 1.00–1.27, P = 0.06). No significant heterogeneity was observed (I2 = 0%).
We then performed a subgroup analysis according to the combination regimens. Overall, the OS did not significantly differ between IRI- and Ox-based regimens in all subgroups (Fig. 3A). The combined therapy of IRI and anti-VEGF was associated with a better PFS (pooled HR = 0.90, 95% CI = 0.82–0.98, P = 0.02), but not with OS (pooled HR = 0.91, 95% CI = 0.80–1.03, P = 0.15) (Fig. 3B and 3A). Ox-based regimens, especially those without molecular targeting agents, were associated with a better ORR (pooled OR = 1.22, 95% CI = 1.03–1.45, P = 0.02) (Fig. 3C).
The incidence of any ≥ grade 3 AEs did not significantly differ between patients who received the two regimens. Thrombocytopenia, peripheral sensory neuropathy, hand–foot syndrome, and allergic reaction were significantly correlated with Ox-based regimens. Meanwhile, leukopenia, diarrhea, and febrile neutropenia were commonly observed in patients who received IRI-based regimens (Fig. 4).
Risk of bias assessment is shown in Fig. 5. Overall, the quality of evidence in this study was moderate according to the risk of bias assessment (Fig. 5A). The funnel plot of each effect size in terms of OS, PFS, and ORR was symmetrical, with a similar number of studies on either side of the summary treatment effect. This result indicated a lack of major publication bias (Fig. 5B).
Based on the current expert panels of guidelines3, 41, 42, there is no preferred regimen that can be used as the initial therapy for mCRC. Hence, IRI- or Ox-based regimen can be an alternative. In clinical practice, the regimen is selected based on efficacy of the regimens, physicians’ experience, and profiles of AEs.
Our analysis showed that there was no significant difference in terms of OS between patients who received IRI- and Ox-based regimens as the first-line treatments for mCRC. This is the first meta-analysis that included treatments containing molecular targeting agents and clinically comparable combination of regimens. Therefore, the results of this study may be more applicable to current clinical practice than those of previous studies. The absence of significant heterogeneity between trials in terms of OS, PFS, and ORR indicated consistent results. Previous reports10–12 showed that Ox-based regimen was more preferred in terms of OS. This discrepancy in results may be attributed to the selection criteria of the trials. That is, previous studies included trials comparing FOLFOX with IFL (bolus 5-FU + IRI) regimen.43, 44 However, Delaunoit et al.45 showed that bolus 5-FU + IRI or Ox could be associated with severe gastrointestinal toxicity and high mortality rates. Thus, excluding these trials was appropriate for the evaluation of efficacy and toxicity between the two regimens.
In the subgroup analysis of regimens without molecular targeting agents, Ox-based regimen was associated with a better ORR. However, the PFS and OS did not significantly differ. In colorectal cancer, the correlation between ORR and OS is not clearly elucidated.46 Hence, our results were not conflicting. In addition, in this subgroup, six of ten trials6, 26–29, 32 used ORR as the primary endpoint, and four6, 27, 29, 32 studies hypothesized that Ox-based regimen is associated with a better ORR. Thus, the evaluation of ORR might be biased in these trials.
In the subgroup analysis of regimens with molecular targeting agents, the combination of anti-VEGF antibody and IRI was more likely to be associated with better PFS and OS. However, the synergic effect of IRI and anti-VEFG antibody had not been reported. Although these data were mainly obtained from Japanese trials7, 39, 40, no data have shown that the combination was more beneficial for Japanese patients. Therefore, we speculated that this result was obtained by chance and was not clinically significant.
With regard to the results of AEs, the incidence of ≥ grade 3 AEs did not significantly differ between patients who received the two regimens. Therefore, it may be reasonable for physicians to select each regimen according to AE profiles. However, Yamazaki et al.7 revealed that the FACT-C OQL score was more likely worse in patients treated with FOLFOX + BEV than in those treated with FOLFIRI + BEV. Moreover, a previous report indicated that peripheral sensory neuropathy lasts for a long period and affects QOL after treatment.47 Thus, physicians should consider QOL during not only the first-line treatment but also the overall survival time when selecting the regimens.
This study had some limitations. That is, it is a meta-analysis. Moreover, there were no data on race, sex, primary site of the tumor, and status of RAS and BRAF genes. Thus, our data must be applied with caution to individual patients in clinical practice. Recently, some reports showed that the molecular subtypes or chromosomal variation of CRC might affect the efficacy of IRI- and Ox-based regimens.48, 49 Thus, in the future, suitable cytotoxic agents should be selected according to biomarker profile.
The efficacy of IRI- and Ox-based regimens when used as the first-line treatments for mCRC did not significantly differ. Hence, both regimens could be used in clinical practice with consideration of the patients’ condition or toxicity profiles.
IRI, irinotecan; Ox, oxaliplatin; mCRC, metastatic colorectal cancer; RCT, randomized controlled trial; OS, overall survival; PFS, progression free survival; ORR, objective response rate; AEs, adverse events; HR, hazard ratio; FPs, fluoropyrimidines; QOL, quality of life; CENTRAL, the Central Registry of Controlled Trials of the Cochrane Library; CI, confidence interval; EGFR, epidermal growth factor receptor; VEGF, vascular endothelial growth factor; CapOx, capecitabine + oxaliplatin; CapIRI, capecitabine + irinotecan; IFL, bolus 5-FU + irinotecan, 5-FU, 5-fluorouracil; BEV, bevacizumab; IRIS, S-1 + irinotecan, FOLFOX and OXAFAFU, 5-FU + folinic acid + oxaliplatin; FOLFIRI and IRIFAFU, 5-FU + folinic acid + irinotecan; TEGAFOX, tegafur + folinic acid + oxaliplatin; TEGAFIRI, tegafur + folinic acid + irinotecan; NA, not available; MTAs, molecular targeting agents
Not applicable. Ethical approval was not required for this study because this meta-analysis is literature based research and did not use individual data.
Not applicable.
All authors declare no conflicts-of-interest related to this article.
The authors have not declared a specific grant for this research from any funding agency in the public, commercial or not-for-profit sectors.
Conceptualization and study design: SK, NT, YH, KY, AN, TK, KM, MY; Writing an original draft: SK; Project administration: YH, KY; Review and editing: SK, NT, YH, AN, MY, TK, KM, KY; Formal analysis: AN, TK, KM; Supervision: YH, KM, KY; Investigation of data: SK, NT, YH, MY; and All authors read and approved the final manuscript.
We would like to show our greatest appreciation to Dr. Goro Nakayama and Dr. Gerardo Rosati for providing data of their clinical trials.
The datasets used and/or analyzed during the current study are available from the corresponding author on reasonable request.