Long-Term Outcomes of Imatinib Treatment for Chronic Myeloid Leukemia

Andreas Hochhaus, Richard A Larson, François Guilhot, Jerald P Radich, Susan Branford, Timothy P Hughes, Michele Baccarani, Michael W Deininger, Francisco Cervantes, Satoko Fujihara, Christine-Elke Ortmann, Hans D Menssen, Hagop Kantarjian, Stephen G O'Brien, Brian J Druker, IRIS Investigators, S Durrant, A Schwarer, D Joske, J Seymour, A Grigg, D Ma, C Arthur, K Bradstock, D Joshua, A Louwagie, P Martiat, N Straetmans, A Bosly, C Shustik, J Lipton, D Forrest, I Walker, D-C Roy, M Rubinger, I Bence-Bruckler, D Stewart, M Kovacs, A R Turner, H Birgens, O Bjerrum, T Facon, J-L Harousseau, M Tulliez, A Guerci, D Blaise, F Maloisel, M Michallet, D Hossfeld, R Mertelsmann, R Andreesen, C Nerl, M Freund, N Gattermann, K Hoeffken, G Ehninger, O Ottmann, C Peschel, S Frühauf, A Neubauer, P Le Coutre, W Aulitzky, R Fanin, G Rosti, F Mandelli, E Morra, A Carella, M Lazzarino, M Petrini, P Rossi Ferrini, F Nobile, V Liso, F Ferrara, V Rizzoli, G Fioritoni, G Martinelli, G Ossenkoppele, P Browett, T Gedde-Dahl, J-M Tangen, I Dahl, J Odriozola, J C Hernández Boluda, J L Steegmann, C Cañizo, A Sureda, J Diaz, A Granena, M N Fernández, L Stenke, C Paul, M Bjoreman, C Malm, H Wadenvik, P-G Nilsson, I Turesson, U Hess, M Solenthaler, J M Goldman, N Russel, G Mufti, J Cavenagh, R E Clark, A R Green, T L Holyoake, G S Lucas, G Smith, D W Milligan, S J Rule, A K Burnett, R Moroose, M Wetzler, J Bearden, R Brown, M Lobell, S Cataland, I Rabinowitz, B Meisenberg, J Gabrilove, K Thompson, S Graziano, P Emanuel, H Gross, P Cobb, R Bhatia, S Dakhil, D Irwin, B Issell, S Pavletic, P Kuebler, E Layhe, P Butera, J Glass, J Moore, B Grant, H Niell, R Herzig, H Burris, B Peterson, B Powell, M Kalaycio, D Stirewalt, W Samlowski, E Berman, S Limentani, T Seay, T Shea, L Akard, G Smith, P Becker, S DeVine, R Hart, R Veith, J Wade, M Brunvand, R Silver, L Kalman, D Strickland, M Shurafa, A Bashey, R Shadduck, S Cooper, H Safah, M Rubenstein, R Collins, A Keller, R Stone, M Tallman, D Stevens, A Pecora, M Agha, H Holmes, B J Druker, F Guilhot, R A Larson, S G O’Brien, J Rowe, C A Schiffer, M Buyse, M Baccarani, F Cervantes, J Cornelissen, T Fischer, A Hochhaus, T Hughes, H Kantarjian, K Lechner, J L Nielsen, J Reiffers, P Rousselot, G Saglio, J Shepherd, B Simonsson, A Gratwohl, K Taylor, G Verhoef, Andreas Hochhaus, Richard A Larson, François Guilhot, Jerald P Radich, Susan Branford, Timothy P Hughes, Michele Baccarani, Michael W Deininger, Francisco Cervantes, Satoko Fujihara, Christine-Elke Ortmann, Hans D Menssen, Hagop Kantarjian, Stephen G O'Brien, Brian J Druker, IRIS Investigators, S Durrant, A Schwarer, D Joske, J Seymour, A Grigg, D Ma, C Arthur, K Bradstock, D Joshua, A Louwagie, P Martiat, N Straetmans, A Bosly, C Shustik, J Lipton, D Forrest, I Walker, D-C Roy, M Rubinger, I Bence-Bruckler, D Stewart, M Kovacs, A R Turner, H Birgens, O Bjerrum, T Facon, J-L Harousseau, M Tulliez, A Guerci, D Blaise, F Maloisel, M Michallet, D Hossfeld, R Mertelsmann, R Andreesen, C Nerl, M Freund, N Gattermann, K Hoeffken, G Ehninger, O Ottmann, C Peschel, S Frühauf, A Neubauer, P Le Coutre, W Aulitzky, R Fanin, G Rosti, F Mandelli, E Morra, A Carella, M Lazzarino, M Petrini, P Rossi Ferrini, F Nobile, V Liso, F Ferrara, V Rizzoli, G Fioritoni, G Martinelli, G Ossenkoppele, P Browett, T Gedde-Dahl, J-M Tangen, I Dahl, J Odriozola, J C Hernández Boluda, J L Steegmann, C Cañizo, A Sureda, J Diaz, A Granena, M N Fernández, L Stenke, C Paul, M Bjoreman, C Malm, H Wadenvik, P-G Nilsson, I Turesson, U Hess, M Solenthaler, J M Goldman, N Russel, G Mufti, J Cavenagh, R E Clark, A R Green, T L Holyoake, G S Lucas, G Smith, D W Milligan, S J Rule, A K Burnett, R Moroose, M Wetzler, J Bearden, R Brown, M Lobell, S Cataland, I Rabinowitz, B Meisenberg, J Gabrilove, K Thompson, S Graziano, P Emanuel, H Gross, P Cobb, R Bhatia, S Dakhil, D Irwin, B Issell, S Pavletic, P Kuebler, E Layhe, P Butera, J Glass, J Moore, B Grant, H Niell, R Herzig, H Burris, B Peterson, B Powell, M Kalaycio, D Stirewalt, W Samlowski, E Berman, S Limentani, T Seay, T Shea, L Akard, G Smith, P Becker, S DeVine, R Hart, R Veith, J Wade, M Brunvand, R Silver, L Kalman, D Strickland, M Shurafa, A Bashey, R Shadduck, S Cooper, H Safah, M Rubenstein, R Collins, A Keller, R Stone, M Tallman, D Stevens, A Pecora, M Agha, H Holmes, B J Druker, F Guilhot, R A Larson, S G O’Brien, J Rowe, C A Schiffer, M Buyse, M Baccarani, F Cervantes, J Cornelissen, T Fischer, A Hochhaus, T Hughes, H Kantarjian, K Lechner, J L Nielsen, J Reiffers, P Rousselot, G Saglio, J Shepherd, B Simonsson, A Gratwohl, K Taylor, G Verhoef

Abstract

Background: Imatinib, a selective BCR-ABL1 kinase inhibitor, improved the prognosis for patients with chronic myeloid leukemia (CML). We conducted efficacy and safety analyses on the basis of more than 10 years of follow-up in patients with CML who were treated with imatinib as initial therapy.

Methods: In this open-label, multicenter trial with crossover design, we randomly assigned patients with newly diagnosed CML in the chronic phase to receive either imatinib or interferon alfa plus cytarabine. Long-term analyses included overall survival, response to treatment, and serious adverse events.

Results: The median follow-up was 10.9 years. Given the high rate of crossover among patients who had been randomly assigned to receive interferon alfa plus cytarabine (65.6%) and the short duration of therapy before crossover in these patients (median, 0.8 years), the current analyses focused on patients who had been randomly assigned to receive imatinib. Among the patients in the imatinib group, the estimated overall survival rate at 10 years was 83.3%. Approximately half the patients (48.3%) who had been randomly assigned to imatinib completed study treatment with imatinib, and 82.8% had a complete cytogenetic response. Serious adverse events that were considered by the investigators to be related to imatinib were uncommon and most frequently occurred during the first year of treatment.

Conclusions: Almost 11 years of follow-up showed that the efficacy of imatinib persisted over time and that long-term administration of imatinib was not associated with unacceptable cumulative or late toxic effects. (Funded by Novartis Pharmaceuticals; IRIS ClinicalTrials.gov numbers, NCT00006343 and NCT00333840 .).

Conflict of interest statement

No other potential conflict of interest relevant to this article was reported.

Figures

Figure 1
Figure 1
Enrollment and Randomization of Patients and Censoring of Data for the Analysis of Overall Survival at 10 Years.
Figure 2. Kaplan–Meier Estimated Overall Survival Rates…
Figure 2. Kaplan–Meier Estimated Overall Survival Rates at 10 Years in the Intention-to-Treat Population
Shown is the overall survival over time among patients assigned to each trial group. For the curve for the group of patients who had been randomly assigned to receive interferon alfa plus cytarabine, data include survival among the 363 patients who crossed over to imatinib (65.6%). These patients crossed over to imatinib after a median of 0.8 years of receiving interferon alfa plus cytarabine. In patients with no reported death (whether because they were known to be alive or because their survival status was unknown), survival was censored (tick marks) at the date of last contact.

Source: PubMed

Sponsoren und Mitarbeiter

Krankheiten

Drogeninterventionen

3
Abonnieren