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MEDITERRANEAN SCHOOL OF ONCOLOGY Ritmi circadiani e qualità di vita: actigrafia e nuovi orizzonti nel carcinoma della mammella Roma, 28 Novembre 2008. Cronomodulazione e farmaci orali. Giuseppe Tonini g.tonini@unicampus.it Oncologia Medica Universita’ Campus Bio-Medico, Roma.
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MEDITERRANEAN SCHOOL OF ONCOLOGY Ritmi circadiani e qualità di vita: actigrafia e nuovi orizzonti nel carcinoma della mammella Roma, 28 Novembre 2008 Cronomodulazione e farmaci orali Giuseppe Tonini g.tonini@unicampus.it Oncologia Medica Universita’ Campus Bio-Medico, Roma
Chronobiology • Chronobiology is the study of the temporal relationships of biological phenomena • Rhythms that fluctuate on a 24-hour time scale are known as circadian rhythms. • The best-known circadian rhythms • body temperature • hormone secretion • metabolism • sleep/wake cycle
Physiology of Circadian Rhythmicity • Prominent daily variations also occur in • endocrine, • thermoregulatory, • cardiac, • pulmonary, • renal, • gastrointestinal, • neurobehavioral functions Harrison
Circadian rhytms in colorectal cancer patients Mormont MC et al, Chronobiol Int 2002
Properties of circadian rythms • Ubiquitous (cyanobacterias, plants, rodents, humans) • Endogenous (persist in the absence of environmental cycles) • Circadian clock genes
In vitro circadian expression of cell cycle genes Delaunay F et al, J Biol Chem 2001
Functional classes of cycling transcripts in cultured rat fibroblasts Delaunay F et al, J Biol Chem 2001
Chronobiology: implications for cancer therapy • Chronotherapy aims to adapt the timing of drug administration according to the circadian rhythms of cancer and normal cells. • Administration of drug at a circadian time when it is best tolerated can achieve best antitumour activity. Mormont and Levi, Cancer 2003
Chronobiology: implications for cancer therapy Circadian rhythms in anticancer drug tolerability in laboratory mice or rats. The least toxic dosing time is indicated as a function of the rest-activity cycle. Mormont and Levi, Cancer 2003
How administer chronotherapy: the multichannel pump • Centralized programmation • Any modulation of delivery rate • 4 reservoirs (100-2000 ml) • Rates from 1 to 3000 ml/h • Safeties • Alarms • Very expensive!!!!
New advances in chronotherapy Phase I, II, III trials are on-going and the results are interesting!!!!
Capecitabine Chronomodulated Capecitabine
Weekly infusion of oxaliplatin • Phase II studies with weekly or biweekly oxaliplatin have demonstrated low levels of toxicity and high clinical activity (Rosati G, Ann Oncol. 2001 and Oncology, 2004; Santini D, Medical Oncology, 2004; Scheithauer W, Ann Oncol, 2003; Kemeny N, Ann Oncol, 2002; Chao Y et al, Br J cancer, 2004) • The weekly oxaliplatin schedule leads to a higher dose-density and a higher total dose administered (Rosati G, Ann Oncol. 2001; Santini D, Medical Oncology, 2004) • The weekly oxaliplatin schedule may lead to a better and more continous synergistic action with capecitabine administered for 14 days
Metastatic colorectal cancer (Folinic Acid, 5-FU, Oxaliplatin) Infusion flow Constant Chrono Toxicity p Oral mucositis gr 3-4 74% 14% <10-4 Neuropathy gr 2-3 31% 16% <10-2 Responding rate 30% 51% <10-3 Toxicity and efficacy of chronomodulated chemotherapy Lévi et al. JNCI 1994 ; Lancet 1997 ; Lancet Onc 2001
Experiences of chronomodulated chemotherapy at Campus Bio-Medico
Continuous infusion of oxaliplatin plus chronomodulated capecitabine in 5-fluorouracil- and irinotecan-resistant advanced colorectal cancer patients. Santini D, Vincenzi B, La Cesa A, Caricato M, Schiavon G, Spalletta B, Di Seri M, Coppola R, Rocci L and Tonini G. Oncology. 2005;69(1):27-34. Chronomodulated administration of oxaliplatin plus capecitabine (XELOX) as first line chemotherapy in advanced colorectal cancer patients: phase II study. Santini D, Vincenzi B, Schiavon G, Di Seri M, Virzi V, Spalletta B, Caricato M, Coppola R and Tonini G. Cancer Chemother Pharmacol. 2007 Apr;59(5):613-20.
181521 8 a.m.-8 p.m. 8 a.m.-8 p.m. X X X C.I. Oxaliplatin (70 mg/mq) Chronomodulated Capecitabine (2000 mg/mq) Treatment scheduleChronomodulated XELOX
Patients characteristics Number of patients (%) 62 (100%) First line 26 Other lines 36 1-2 previous lines 16-20 Median age, years (range) 65 (32-77) Male/Female 32/30 ECOG 0/1/2 36/22/4 Colon/rectal (%) 68/32 Single/> 1 metastatic sites (%) 48/52 >2 metastatic sites(%) 27.1% Metastatic sites (%) liver /lung 68.7/47.9
Best confirmed responses in first line chemotherapy (% patients)
Best confirmed responses in other lines of chemotherapy (% patients) N Pts (%) 36 (100%) CR 0 (0%) PR 11 (30.6%) SD 13 (36.1%) PD 12 (33.3%) CR-PR 11 (30.6%) Disease stabilization 24 (66.6%) (CR-PR-SD)
Survival data in first line chemotherapy N Pts 26 Months (95% C.I.) Progression free survival 9.66 (6.88 - 12.45) Median survival 19.74 (15.92–23.56) 1-year survival rate 84.6% (22 Pts)
Survival data in other lines of chemotherapy N Pts 36 Months (range) Progression free survival 6.7 (4.9-8.4) Median survival 11.3 (6.6-13.1) 1-year survival rate 53.8%
Safety results (after dose reduction) toxicity per patient (47 patients) NCI Gr 3 % patients Thrombocytopenia 0 Neutropenia 6.1 Febrile neutropenia 0 Anemia 0 Asthenia 21.2 Diarrhea 12.1 Stomatitis 3 Vomiting 6.1 Hand foot syndrome 3.0 Alopecia (Gr2) 3.0 Liver 3.0
Conclusions With high activity and good tolerability, chronomodulated XELOX compares favorably with standard XELOX • High RR% in first and other lines • TTP in first line comparable with the best schedules • Favorable median survival • Responses in oxaliplatin-pretreated patients • Low incidence of severe neurotoxicity and hand foot syndrome • Low incidence of severe diarrhea after dose reduction of capecitabine
Bevacizumab plus chronomodulated capecitabine as first-line advanced colorectal cancer patients. (Unpublished data)
Schedule • Oxaliplatin: 70m/mq (gg 1-8q21) • Bevacizumab: 7,5 mg/mq (gg1q21) • Capecitabine: 1750 mg/mq (gg1-14q21): ¼ h 8, ¼ h 18, ½ h 23.
Phase I study of intermittent and chronomodulated oral therapy with capecitabine in patients with advanced and/or metastatic cancer. Santini D, Vincenzi B, Schiavon G, La Cesa A, Gasparro S, Vincenzi A and Tonini G. BMC Cancer. 2006; 24;6:42
Schedules and end-points Schedule: Capecitabine 1500-2750 mg/mq (gg1-14q21): ¼ h 8, ¼ h 18, ½ h 23. Endpoints: • Maximum-tolerated dose • Dose-limiting toxicities • Safety
Results • Most common toxicities: fatigue, diarrhoea and hand foot syndrome. • Only 1/9 pts treated at capecitabine dose of 2,750 mg/m2 had DLT toxicities (fatigue G4). • No other episodes of DLT were observed at the same dose steps and at lower doses of capecitabine. • The dose of 2,750 mg/m2 is recommended for further study. • Tumor responses were observed in patients with metastatic breast (6 PR) and colorectal cancer (3 PR).
Conclusions • Circadian rhythms modulate cell functions relevant for: - anticancer agent pharmacology - Cancer processes • New advances in cancer chronotherapy : • Programmable drug delivery devices • Relevance shown in Phase I, II & III clinical trials
Conclusions • In our experience chronomodulated chemotherapy is effective and well tolerated • Our results clearly highlight the need for new trials to verify the real clinical impact of this new way of chronomodulated capecitabine administration in combination with other active drugs in solid tumors.
Oncologia Medica Università Campus Bio-Medico, Roma Giuseppe Tonini Daniele Santini Francesco Pantano Bruno Vincenzi Maria Elisabetta Fratto Annalisa La Cesa Alice Calvieri Claudia Grilli Olga Venditti Sara Galluzzo Chiara Spoto Simona Gasparro Salvatore Intagliata Vladimir Virzì Calogero Gucciardino Gaia Schiavon Laura Rocci Valentina Leoni Federica Uzzalli Marianna Silletta Marzia Mazzaroni