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Safety and efficacy of STI-571 (imatinib mesylate) in patients with bcr/abl-positive chronic myelogenous leukemia (CML) after autologous peripheral blood stem cell transplantation (PBSCT)

Safety and efficacy of STI-571 (imatinib mesylate) in patients with bcr/abl-positive chronic myelogenous leukemia (CML) after autologous peripheral blood stem cell transplantation (PBSCT)
Safety and efficacy of STI-571 (imatinib mesylate) in patients with bcr/abl-positive chronic myelogenous leukemia (CML) after autologous peripheral blood stem cell transplantation (PBSCT)
We examined safety and efficacy of STI-571 in 24 bcr/abl-positive patients with CML post PBSCT. At start of STI-571 therapy, nine patients presented in blast crisis (BC) or in accelerated phase (AP), and 15 in chronic phase (CP). Patients were evaluated for hematologic, cytogenetic and molecular response, survival and toxicity. In general, STI-571 was well tolerated in this heavily pretreated group of patients with a non-hematologic and hematologic toxicity profile similar to that observed in a previous phase I trial at comparable doses. Five of nine patients with CML in transformation (AP, BC) were evaluable for hematologic response. Two of five patients had transient reductions in WBC and blasts, and three patients achieved a sustained hematologic response (>4 weeks). Cytogenetic analysis in these patients revealed numerical and/or structural responses. In CML chronic phase, STI-571 induced complete hematologic responses in all patients and major cytogenetic responses in 61% of patients with a complete cytogenetic response rate of 46%. This report indicates that STI-571 is a safe and effective drug in heavily pretreated patients. No apparent additional side-effects were noted in this patient cohort. The high rate of complete hematologic and complete cytogenetic responses in CP patients is remarkable, as intensive treatment approaches plus IFN-alpha failed to be efficient in achieving long-term stabilization of CML in this patient cohort.
0887-6924
1220 -1228
Fischer, T.
aba70ee0-35f0-416e-a436-658edcd9b1eb
Reifenrath, C.
50744edf-6112-4adc-97e8-fd7ff6995c4c
Hess, G. R.
409c03b1-29a9-403a-8cdd-d174ffe1fa55
Corsetti, M. T.
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Kreil, S.
2404ac13-cdaa-43a3-913b-adceb79e598f
Beck, J.
8246ed92-e608-420b-ad57-7a0fdcfe0b9d
Meinhardt, P.
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Beltrami, G.
51f9e6dc-3427-46c5-a585-cebb35b57647
Schuch, B.
cce98a25-3fba-42e9-85c5-e9cf2913632a
Gschaidmeier, H.
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Hehlmann, R.
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Hochhaus, A.
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Carella, A.
eb4b0ecc-8881-44f2-9e2b-6d223b11915c
Huber, C.
7dbee735-9f93-4abe-abae-481c72d4d1a1
Fischer, T.
aba70ee0-35f0-416e-a436-658edcd9b1eb
Reifenrath, C.
50744edf-6112-4adc-97e8-fd7ff6995c4c
Hess, G. R.
409c03b1-29a9-403a-8cdd-d174ffe1fa55
Corsetti, M. T.
1026f0df-e11c-4684-85f1-f01e27e3f122
Kreil, S.
2404ac13-cdaa-43a3-913b-adceb79e598f
Beck, J.
8246ed92-e608-420b-ad57-7a0fdcfe0b9d
Meinhardt, P.
3f5444a7-9a3f-4a70-8ee8-2ba7bf6f7a19
Beltrami, G.
51f9e6dc-3427-46c5-a585-cebb35b57647
Schuch, B.
cce98a25-3fba-42e9-85c5-e9cf2913632a
Gschaidmeier, H.
46d97d80-f9c6-4286-af8a-407d4a282058
Hehlmann, R.
753d719b-7bf8-4f74-bfdc-6d5d47e5d2c7
Hochhaus, A.
4c0b9da4-adfa-4253-8af7-78cec9e9a24f
Carella, A.
eb4b0ecc-8881-44f2-9e2b-6d223b11915c
Huber, C.
7dbee735-9f93-4abe-abae-481c72d4d1a1

Fischer, T., Reifenrath, C., Hess, G. R., Corsetti, M. T., Kreil, S., Beck, J., Meinhardt, P., Beltrami, G., Schuch, B., Gschaidmeier, H., Hehlmann, R., Hochhaus, A., Carella, A. and Huber, C. (2002) Safety and efficacy of STI-571 (imatinib mesylate) in patients with bcr/abl-positive chronic myelogenous leukemia (CML) after autologous peripheral blood stem cell transplantation (PBSCT). Leukemia, 16 (7), 1220 -1228. (doi:10.1038/sj.leu.2402565).

Record type: Article

Abstract

We examined safety and efficacy of STI-571 in 24 bcr/abl-positive patients with CML post PBSCT. At start of STI-571 therapy, nine patients presented in blast crisis (BC) or in accelerated phase (AP), and 15 in chronic phase (CP). Patients were evaluated for hematologic, cytogenetic and molecular response, survival and toxicity. In general, STI-571 was well tolerated in this heavily pretreated group of patients with a non-hematologic and hematologic toxicity profile similar to that observed in a previous phase I trial at comparable doses. Five of nine patients with CML in transformation (AP, BC) were evaluable for hematologic response. Two of five patients had transient reductions in WBC and blasts, and three patients achieved a sustained hematologic response (>4 weeks). Cytogenetic analysis in these patients revealed numerical and/or structural responses. In CML chronic phase, STI-571 induced complete hematologic responses in all patients and major cytogenetic responses in 61% of patients with a complete cytogenetic response rate of 46%. This report indicates that STI-571 is a safe and effective drug in heavily pretreated patients. No apparent additional side-effects were noted in this patient cohort. The high rate of complete hematologic and complete cytogenetic responses in CP patients is remarkable, as intensive treatment approaches plus IFN-alpha failed to be efficient in achieving long-term stabilization of CML in this patient cohort.

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Published date: 2002

Identifiers

Local EPrints ID: 24699
URI: http://eprints.soton.ac.uk/id/eprint/24699
ISSN: 0887-6924
PURE UUID: 8214aece-e8a2-4fb1-8954-df88f6794413

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Date deposited: 03 Apr 2006
Last modified: 15 Mar 2024 06:57

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Contributors

Author: T. Fischer
Author: C. Reifenrath
Author: G. R. Hess
Author: M. T. Corsetti
Author: S. Kreil
Author: J. Beck
Author: P. Meinhardt
Author: G. Beltrami
Author: B. Schuch
Author: H. Gschaidmeier
Author: R. Hehlmann
Author: A. Hochhaus
Author: A. Carella
Author: C. Huber

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