Sex‐dependent least toxic timing of irinotecan combined with chronomodulated chemotherapy for metastatic colorectal cancer: Randomized multicenter EORTC 05011 trial
Abstract The least toxic time (LTT) of irinotecan varied by up to 8 hours according to sex and genetic background in mice. The translational relevance was investigated within a randomized trial dataset, where no LTT stood out significantly in the whole population. 130 male and 63 female eligible pat...
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2020-06-01
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| Series: | Cancer Medicine |
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| Online Access: | https://doi.org/10.1002/cam4.3056 |
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doaj-2990600537df42ceb50e3ef287e9b4672020-11-25T02:24:20ZengWileyCancer Medicine2045-76342020-06-019124148415910.1002/cam4.3056Sex‐dependent least toxic timing of irinotecan combined with chronomodulated chemotherapy for metastatic colorectal cancer: Randomized multicenter EORTC 05011 trialPasquale F. Innominato0Annabelle Ballesta1Qi Huang2Christian Focan3Philippe Chollet4Abdoulaye Karaboué5Sylvie Giacchetti6Mohamed Bouchahda7René Adam8Carlo Garufi9Francis A. Lévi10North Wales Cancer CentreBetsi Cadwaladr University Health Board Bangor United KingdomDivision of Biomedical Sciences Cancer Chronotherapy TeamCancer Research CentreWarwick Medical School Coventry United KingdomDivision of Biomedical Sciences Cancer Chronotherapy TeamCancer Research CentreWarwick Medical School Coventry United KingdomDepartment of Oncology Clinique Saint‐JosephCHC‐Liège Hospital Group Liège BelgiumClinical and Translational Research Division Jean Perrin Comprehensive Cancer Centre Clermont‐Ferrand FranceMedical Oncology Unit GHI Le Raincy‐Montfermeil Montfermeil FranceUMRS 935, "Cancer Chronotherapy and Postoperative Liver Functions" French National Institute for Health and Medical Research (INSERM) and Paris‐Sud University Villejuif FranceUMRS 935, "Cancer Chronotherapy and Postoperative Liver Functions" French National Institute for Health and Medical Research (INSERM) and Paris‐Sud University Villejuif FranceUMRS 935, "Cancer Chronotherapy and Postoperative Liver Functions" French National Institute for Health and Medical Research (INSERM) and Paris‐Sud University Villejuif FranceDivision of Medical Oncology San Camillo Forlanini Hospital Roma ItalyDivision of Biomedical Sciences Cancer Chronotherapy TeamCancer Research CentreWarwick Medical School Coventry United KingdomAbstract The least toxic time (LTT) of irinotecan varied by up to 8 hours according to sex and genetic background in mice. The translational relevance was investigated within a randomized trial dataset, where no LTT stood out significantly in the whole population. 130 male and 63 female eligible patients with metastatic colorectal cancer were randomized to receive chronomodulated Irinotecan with peak delivery rate at 1 of 6 clock hours staggered by 4 hours on day 1, then fixed‐time chronomodulated Fluorouracil‐Leucovorin‐Oxaliplatin for 4 days, q3 weeks. The sex‐specific circadian characteristics of grade (G) 3‐4 toxicities were mapped with cosinor and time*sex interactions confirmed with Fisher's exact test. Baseline characteristics of male or female patients were similar in the six treatment groups. Main grade 3‐4 toxicities over six courses were diarrhea (males vs females, 39.2%; vs 46.0%), neutropenia (15.6% vs 15.0%), fatigue (11.5% vs 15.9%), and anorexia (10.0% vs 7.8%). They were reduced following irinotecan peak delivery in the morning for males, but in the afternoon for females, with statistically significant rhythms (P < .05 from cosinor) and sex*timing interactions (Fisher's exact test, diarrhea, P = .023; neutropenia, P = .015; fatigue, P = .062; anorexia, P = .032). Irinotecan timing was most critical for females, with grades 3‐4 ranging from 55.2% of the patients (morning) to 29.4% (afternoon) for diarrhea, and from 25.9% (morning) to 0% (afternoon) for neutropenia. The study results support irinotecan administration in the morning for males and in the afternoon for females, in order to minimize adverse events without impairing efficacy.https://doi.org/10.1002/cam4.3056chronotherapycircadiancolorectal cancergenderirinotecantoxicity |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Pasquale F. Innominato Annabelle Ballesta Qi Huang Christian Focan Philippe Chollet Abdoulaye Karaboué Sylvie Giacchetti Mohamed Bouchahda René Adam Carlo Garufi Francis A. Lévi |
| spellingShingle |
Pasquale F. Innominato Annabelle Ballesta Qi Huang Christian Focan Philippe Chollet Abdoulaye Karaboué Sylvie Giacchetti Mohamed Bouchahda René Adam Carlo Garufi Francis A. Lévi Sex‐dependent least toxic timing of irinotecan combined with chronomodulated chemotherapy for metastatic colorectal cancer: Randomized multicenter EORTC 05011 trial Cancer Medicine chronotherapy circadian colorectal cancer gender irinotecan toxicity |
| author_facet |
Pasquale F. Innominato Annabelle Ballesta Qi Huang Christian Focan Philippe Chollet Abdoulaye Karaboué Sylvie Giacchetti Mohamed Bouchahda René Adam Carlo Garufi Francis A. Lévi |
| author_sort |
Pasquale F. Innominato |
| title |
Sex‐dependent least toxic timing of irinotecan combined with chronomodulated chemotherapy for metastatic colorectal cancer: Randomized multicenter EORTC 05011 trial |
| title_short |
Sex‐dependent least toxic timing of irinotecan combined with chronomodulated chemotherapy for metastatic colorectal cancer: Randomized multicenter EORTC 05011 trial |
| title_full |
Sex‐dependent least toxic timing of irinotecan combined with chronomodulated chemotherapy for metastatic colorectal cancer: Randomized multicenter EORTC 05011 trial |
| title_fullStr |
Sex‐dependent least toxic timing of irinotecan combined with chronomodulated chemotherapy for metastatic colorectal cancer: Randomized multicenter EORTC 05011 trial |
| title_full_unstemmed |
Sex‐dependent least toxic timing of irinotecan combined with chronomodulated chemotherapy for metastatic colorectal cancer: Randomized multicenter EORTC 05011 trial |
| title_sort |
sex‐dependent least toxic timing of irinotecan combined with chronomodulated chemotherapy for metastatic colorectal cancer: randomized multicenter eortc 05011 trial |
| publisher |
Wiley |
| series |
Cancer Medicine |
| issn |
2045-7634 |
| publishDate |
2020-06-01 |
| description |
Abstract The least toxic time (LTT) of irinotecan varied by up to 8 hours according to sex and genetic background in mice. The translational relevance was investigated within a randomized trial dataset, where no LTT stood out significantly in the whole population. 130 male and 63 female eligible patients with metastatic colorectal cancer were randomized to receive chronomodulated Irinotecan with peak delivery rate at 1 of 6 clock hours staggered by 4 hours on day 1, then fixed‐time chronomodulated Fluorouracil‐Leucovorin‐Oxaliplatin for 4 days, q3 weeks. The sex‐specific circadian characteristics of grade (G) 3‐4 toxicities were mapped with cosinor and time*sex interactions confirmed with Fisher's exact test. Baseline characteristics of male or female patients were similar in the six treatment groups. Main grade 3‐4 toxicities over six courses were diarrhea (males vs females, 39.2%; vs 46.0%), neutropenia (15.6% vs 15.0%), fatigue (11.5% vs 15.9%), and anorexia (10.0% vs 7.8%). They were reduced following irinotecan peak delivery in the morning for males, but in the afternoon for females, with statistically significant rhythms (P < .05 from cosinor) and sex*timing interactions (Fisher's exact test, diarrhea, P = .023; neutropenia, P = .015; fatigue, P = .062; anorexia, P = .032). Irinotecan timing was most critical for females, with grades 3‐4 ranging from 55.2% of the patients (morning) to 29.4% (afternoon) for diarrhea, and from 25.9% (morning) to 0% (afternoon) for neutropenia. The study results support irinotecan administration in the morning for males and in the afternoon for females, in order to minimize adverse events without impairing efficacy. |
| topic |
chronotherapy circadian colorectal cancer gender irinotecan toxicity |
| url |
https://doi.org/10.1002/cam4.3056 |
| work_keys_str_mv |
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