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December 2002, Volume 16, Number 12, Pages 2366-2378
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Original Manuscript
Pooled analysis of clinical and cytogenetic features in treatment-related and de novo adult acute myeloid leukemia and myelodysplastic syndromes based on a consecutive series of 761 patients analyzed 1976-1993 and on 5098 unselected cases reported in the literature 1974-2001
N Mauritzson1, M Albin2, L Rylander2, R Billström1, T Ahlgren3, Z Mikoczy2, J Björk2, U Strömberg2, P G Nilsson1, F Mitelman4, L Hagmar2 and B Johansson4

1Department of Hematology, Lund University Hospital, Sweden

2Department of Occupational and Environmental Medicine, Lund University Hospital, Sweden

3Department of Hematology, Malmö University Hospital, Sweden

4Department of Clinical Genetics, Lund University Hospital, Sweden

Correspondence to: N Mauritzson, Department of Hematology, University Hospital, SE-221 85 Lund, Sweden; Fax: 46 46 211 0908

Abstract

To ascertain the frequency of treatment-related acute myeloid leukemias and myelodysplastic syndromes (t-AML/t-MDS) in an unselected series, we have identified all adult cases analyzed in our department from 1976 to 1993. Further aims were to compare karyotypic features of t-AML/t-MDS with de novo AML/MDS, in our material as well as in 5098 unselected, cyto- genetically abnormal, published cases, and to analyze associations between type of prior therapy and karyotype. Among our 372 AML and 389 MDS, 47 (13%) were t-AML and 62 (16%) were t-MDS. Clonal abnormalities were significantly more common in t-AML and t-MDS than in de novo disease (68% vs 50%, P < 0.05 and 84% vs 45%, P < 0.001, respectively). Among the available 4230 AML and 1629 MDS (the present series and published cases), 14% were t-AML and 15% were t-MDS. In t-AML/t-MDS, the number of anomalies and the ploidy levels differed significantly from de novo cases, with complex and hypodiploid karyotypes being more common in t-AML/t-MDS. In t-AML, unbalanced changes in general, t(1;3), der(1;7), 3p-, -5, 5q-, -7, 7q-, t(9;11), t(11;19), t(11q23), der(12p), -17, der(17p), -18, and -21 were significantly more frequent than in de novo AML. In t-MDS, -5, -7, 7q-, 13q-, der(17p), and -18 were significantly more common. Type of prior treatment correlated significantly with number of anomalies in t-AML and with ploidy levels in t-AML/t-MDS. The frequencies of several aberrations varied with type of therapy, eg, 5q- was more frequent in radiotherapy-associated t-MDS, monosomy 7 was more common in t-AML and t-MDS after treatment with alkylators, and t(11q23) in t-AML was associated with topoisomerase II inhibitors. Abnormalities significantly more common in de novo disease were +8 as a sole anomaly, balanced changes in general, t(8;21), t(9;22), t(15;17), inv(16), and t(21q22) in AML, and -Y, 5q-, and 20q- as sole anomalies and +8 in MDS. The results emphasize the strong association between previous genotoxic exposure and karyotypic features.

Leukemia (2002) 16, 2366-2378. doi:10.1038/sj.leu.2402713

Keywords

treatment-related; acute myeloid leukemia; myelodysplastic syndromes; karyotype

Received 14 December 2001; accepted 26 June 2002
December 2002, Volume 16, Number 12, Pages 2366-2378
Table of contents    Previous  Abstract  Next   Full text  PDF
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