par Van Cutsem, Eric;Dirix, Luc Y;Van Laethem, Jean-Luc 
;Van Belle, Simon;Borner, Markus;Gonzalez Baron, M.;Roth, A.;Morant, Rudolf;Joosens, E;Gruia, Gabriela;Sibaud, D.;Bleiberg, Harry
Référence British Journal of Cancer, 92, 6, page (1055-1062)
Publication Publié, 2005-03
;Van Belle, Simon;Borner, Markus;Gonzalez Baron, M.;Roth, A.;Morant, Rudolf;Joosens, E;Gruia, Gabriela;Sibaud, D.;Bleiberg, Harry Référence British Journal of Cancer, 92, 6, page (1055-1062)
Publication Publié, 2005-03
Article révisé par les pairs
| Résumé : | Although irinotecan 350 mg m(-2) is a standard option for relapsed/refractory advanced colorectal cancer, there is some evidence that suggests that a higher dose may be more effective, with acceptable tolerability, following 5-fluorouracil (5-FU). This study assessed the optimal dosing strategy for irinotecan, along with treatment efficacy and safety. A total of 164 patients with metastatic colorectal cancer progressing after failure on 5-FU or raltitrexed received either 350 mg m(-2) irinotecan (Group A; n=36) or 250, 350 or 500 mg m(-2), according to individual patient tolerance (Group B; n=62) or based on risk factor optimisation (Group C; n=66). There were no complete responses. There was a trend towards a higher overall response rate in Group B (13%) than in Groups A (8%) and C (9%). Tumour control growth rate was high in all three groups: 58% in group A, 60% in Group B and 50% in Group C. A total of 34% of patients in Group B and 9% in Group C were able to receive a dose of 500 mg m(-2). Median duration of response and time to progression were significantly longer in Groups A and B compared with Group C. No significant between-group differences for any adverse events were seen, although there was a small trend towards better tolerability in Group B. Individual dose escalation based on patient tolerance may allow more patients to receive a higher irinotecan dose without causing additional toxicity and can be an appropriate patient management strategy. |
