3 versus 6 months of adjuvant oxaliplatin-fluoropyrimidine combination therapy for colorectal cancer (SCOT): an international, randomised, phase 3, non-inferiority trial

Iveson, Tim; Kerr, David J.; Saunders, Mark; Cassidy, Jim; Holländer, Niels Henrik; Tabernero, Josep; Haydon, Andrew; Glimelius, Bengt; Harkin, Andrea; Allan, Karen; McQueen, John; Scudder, Claire; Boyd, Kathleen; Briggs, Andrew; Waterston, Ashita; Medley, Louise; Wilson, Charles B.; Ellis, Richard; Essapen, Sharadah; Dhadda, A.S.; Harrison, Mark; Falk, Stephen; Raouf, Sherif; Rees, Charlotte; Olesen, René K; Propper, David; Bridgewater, John; Azzabi, Ashraf; Farrugia, David; Webb, Andrew R.; Cunningham, David; Hickish, Tamas; Weaver, Andrew; Gollins, Simon; Wasan, Harpreet; Paul, James

doi:10.1016/s1470-2045(18)30093-7

Cited by 150 publications

(199 citation statements)

References 26 publications

(33 reference statements)

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“…The risk of long-term neuropathy has been associated with cumulative dose of oxaliplatin in some studies [13,26,27], but not in all [12,28]. In the three registration studies, less neuropathy was noted in the study with 25% lower cumulative dose [4,6].…”

Section: Discussionmentioning

confidence: 97%

Long-term neuropathy and quality of life in colorectal cancer patients treated with oxaliplatin containing adjuvant chemotherapy

Soveri

Lamminmäki²,

Hänninen

et al. 2019

Acta Oncologica

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Background: Oxaliplatin, combined with capecitabine (CAPOX) or infused 5-fluorouracil (FOLFOX), is standard of care in the adjuvant treatment of colorectal cancer (CRC). Prospective data on prevalence of oxaliplatin induced acute and long-term neuropathy in a real-life patient population and its effects on quality of life (QOL) and survival is limited, and scarce in CAPOX versus FOLFOX treated, especially in a subarctic climate. Methods: One hundred forty-four adjuvant CRC patients (all 72 CAPOX cases and 72 matched FOLFOX controls) were analyzed regarding oxaliplatin induced sensory neuropathy, which was graded according to NCI-CTCAEv3.0. Ninety-two long-term survivors responded to the QOL (EORTC QLQ-C30) and Chemotherapy-Induced Peripheral Neuropathy (EORTC CIPN20) questionnaires and were interviewed regarding long-term neuropathy. Results: Acute neurotoxicity was present in 94% (136/144) during adjuvant therapy and there was a significant association between acute neurotoxicity and long-term neuropathy (p < .001). Long-term neuropathy was present in 69% (grade 1/2/3/4 in 36/24/8/1%) at median 4.2 years. Neuropathy grades 2-4 did not influence global health status, but it was associated with decreased physical functioning (p ¼ .031), decreased role functioning (p ¼ .040), and more diarrhea (p ¼ .021) in QLQ-C30 items. There were no differences in acute neurotoxicity, long-term neuropathy, or in QOL between CAPOX and FOLFOX treated. Neuropathy showed no pattern of variation according to starting and stopping month or treatment during winter. Conclusions: Neuropathy following oxaliplatin containing adjuvant chemotherapy is present in twothirds, years after cessation, and impairs some QOL scales. There is no difference in severity of acute or long-term neuropathy between CAPOX and FOLFOX treated and QOL is similar. No seasonal variation in neuropathy was noted.

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Section: Discussionmentioning

confidence: 97%

Long-term neuropathy and quality of life in colorectal cancer patients treated with oxaliplatin containing adjuvant chemotherapy

Soveri

Lamminmäki²,

Hänninen

et al. 2019

Acta Oncologica

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“…Our ndings from population-based cancer registry data con rmed that higher chemotherapy RDI was needed in high-risk stage III colon cancers, compared with low-risk cancers, and are consistent with the conclusions from six randomized, phase 3 clinical trials conducted by the International Duration Evaluation of Adjuvant Therapy (IDEA) collaboration, which found that 6 months of FOLFOX particularly bene ted high-risk stage III colon cancers. These clinical trials evaluated whether 3 months of FOLFOX or CAPOX is non-inferior to 6 months of therapy in the rate of disease-free survival at 3 years [4,9,32,33]. Results from a pooled analysis of six trials showed that in stage III colon cancer patients treated with FOLFOX, 6-month therapy had a higher rate of disease-free survival than 3-month therapy, particularly in the high-risk group [9].…”

Section: Discussionmentioning

confidence: 99%

Impact of relative dose intensity of FOLFOX adjuvant chemotherapy on risk of death among stage III colon cancer patients

Zhou

Thompson²,

Lin

et al. 2020

Preprint

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Background: Clinical trials have suggested high-risk (T4 and/or N2) and low-risk (T1-T3 and N1) stage III colon cancer patients might need different doses of FOLFOX to reserve a similar survival probability. Observational studies have investigated the effect of relative dose intensity (RDI) of FOLFOX on cancer survival for patients with stage III colon cancer, but nonetheless, the studies focused on very specific populations, and none performed stratified analysis by risk profiles. This study aims to identify the optimal RDI of FOLFOX administered for high-risk and low-risk stage III colon cancer patients. Methods: Data on 407 eligible patients, diagnosed with stage III colon cancer in 2011 who received FOLFOX, were collected by the eight population-based cancer registries for a CDC National Program of Cancer Registries (NPCR) project focused on Comparative Effectiveness Research. We employed Kaplan-Meier method, cumulative incidence function (CIF), Multivariable Cox model and Fine-Gray competing risks model to explore Optimal RDI defined as the lowest RDI administered without significant differences in either overall or cause-specific death. Results: Among the 168 high-risk patients, the optimal RDI cut-off point was 70% where there was no statistically significant difference in overall mortality (HR=1.59; 95% CI: 0.69-3.66) and cause-specific mortality (HR=1.24; 95% CI: 0.42-3.64) when RDI<70% vs. RDI≥70%, adjusting for sociodemographic and clinical covariates. When the RDI cut-off was lower than the optimal one (<55% vs. ≥55%, <60% vs. ≥60%, or <65% vs. ≥65%), the overall mortality was significantly statistically different between the two groups of each comparison. Among the 239 low-risk patients, none of the evaluated cut-offs were associated with statistically significant differences in overall and cause-specific mortalities between comparison groups. The lowest RDI we assessed was 45%, HR=0.80; 95% CI: 0.24-2.73 for the overall mortality and HR=0.53; 95% CI: 0.06-4.95 for the cause-specific mortality, when RDI<45% vs. RDI≥45%. Conclusions: To best utilize health care resources while maintaining efficacy, RDI can be maintained at a minimum of 70% for high-risk stage III colon cancer patients. For low-risk patients, we found that RDI as low as 45% did not significantly affect the risk of death.

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“…In one of the trials comparing 3 vs 6 months of adjuvant FOLFOX or CAPOX, the SCOT trial [11], another patientreported outcome measure than CIPN20, used by Soveri et al [9], the FACT/GOG NTx-4 scale was used. The scores in the 6-month arm (approximately 60% of patients actually received 6 months oxaliplatin) were about twice as high as in the 3-month arm (approximately 85% received 3 months), showing that longer treatment gives more acute and late neurotoxicity.…”

Section: How Much Less Is Seen If 3 Months Of Oxaliplatin Is Given?mentioning

confidence: 99%

“…In the adjuvant setting, two aspects will decrease the use of oxaliplatin. One, and the reason most clinicians likely first think of, is, as described above, the recently reported trials revealing that 3 months of oxaliplatin-containing chemotherapy is for many patients not inferior to 6 months of therapy and that the shorter treatment results in less OIPN [10,11,14]. Since the release of trial data in the spring 2018 and the full publications later in 2018, the duration of adjuvant oxaliplatin-containing treatment has likely been shortened worldwide for many, if not all patients.…”

Section: How Much Less Is Seen If 3 Months Of Oxaliplatin Is Given?mentioning

confidence: 99%

“…Controversies still exist about whether the two schedules, CAPOX or FOLFOX should be handled differently and for what subgroups, if any, the reference treatment still is 6 months. According to a substudy of the SCOT trial [11], the largest of the 5 trials in the IDEA consortium [10], 6 months of therapy is never costeffective [15]. It is beyond the purpose of this editorial to discuss pros and cons of 3 or 6 months of adjuvant therapy, but the clinical problem of long-lasting OIPN will diminish as a result of the practice changing 3 vs 6 months adjuvant trials.…”

Section: How Much Less Is Seen If 3 Months Of Oxaliplatin Is Given?mentioning

confidence: 99%

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Lessons learned from the maturation of a cancer drug: oxaliplatin in colorectal cancer

Glimelius

Nygren

2019

Acta Oncologica

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The addition of oxaliplatin to a fluoropyrimidine is reference treatment after colon cancer surgery in patients with stage III and in stage II if at least one high-risk criterium for recurrence is present [1-3]. Even if guidelines open for using a fluoropyrimidine alone, there is a tendency to add oxaliplatin whenever adjuvant chemotherapy is indicated, at least in stage III. Three randomized trials comparing adjuvant therapy for six months using a fluoropyrimidine with or without oxaliplatin showed that the combination improved disease-free survival (DFS) by approximately 20% (hazard ratios, HRs 0.80-0.82) [4-6]. Overall survival was also slightly improved (HRs 0.84-0.88). An average risk of recurrence of 30% after fluoropyrimidine treatment alone, typical for many stage III patients, means that six additional patients per 100 treated will not experience any recurrence if oxaliplatin was added. If the recurrence risk is higher, more treated patients are gained, but for many stage III patients, including most patients with stage II and high-risk criteria, the recurrence risk is less, and the gain from adding oxaliplatin is only a few percent. All treated patients are at risk of toxicity, including the oxaliplatin-induced chronic and often disabling neurotoxicity. The oxaliplatin-induced peripheral neuropathy (OIPN) was considered along with the gains in recurrence risk and survival when different scientific and clinical organizations such as ASCO and NCCN in the US and ESMO in Europe and national groups recommended an oxaliplatin combination for all stage III colon cancers and for stage II cancers with high-risk factors. The extent of the adverse effects, i.e. the downside of adding oxaliplatin was known from the clinical trials where the treating physicians graded the neurotoxicity according to one of a few recommended scales. Typically, acute peripheral neurotoxicity of grade 2 or higher was recorded in 30-50% of the patients and although chronic OIPN was seen, it was not considered extensive [4-6]. In the MOSAIC trial, grade 2 and 3 chronic neuropathy were seen in 4.8 and 1.3%, respectively, after 12 months and in 3.4 and 0.7%, respectively, after 4 years [4].

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3 versus 6 months of adjuvant oxaliplatin-fluoropyrimidine combination therapy for colorectal cancer (SCOT): an international, randomised, phase 3, non-inferiority trial

Cited by 150 publications

References 26 publications

Long-term neuropathy and quality of life in colorectal cancer patients treated with oxaliplatin containing adjuvant chemotherapy

Long-term neuropathy and quality of life in colorectal cancer patients treated with oxaliplatin containing adjuvant chemotherapy

Impact of relative dose intensity of FOLFOX adjuvant chemotherapy on risk of death among stage III colon cancer patients

Lessons learned from the maturation of a cancer drug: oxaliplatin in colorectal cancer

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