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Molecular cytogenetic study of derivative chromosome 9 deletion in chronic myeloid leukemia patients
Authors:Ayda Bennour  Ines Ouahchi  Yosra Ben Youssef  Monia Zaier  Mohamed Adnéne Laatiri  Imed Harrabi  Balkis Meddeb  Moez Elloumi  Abderrahim Khelif  Ali Saad  Halima Sennana
Institution:1. Department of Cytogenetics, Molecular Genetics and Reproductive Biology, Farhat Hached University Teaching Hospital, Sousse, Tunisia
2. Department of Clinical Hematology, Farhat Hached University Teaching Hospital, Sousse, Tunisia
3. Department of Clinical Hematology, Fattouma Bourguiba University Teaching Hospital, Monastir, Tunisia
4. Department of Epidemiology and Medical Statistics, Farhat Hached University Teaching Hospital, Sousse, Tunisia
5. Department of Clinical Hematology, Aziza Othmana University Teaching Hospital, Tunis, Tunisia
6. Department of Clinical Hematology, Hedi Chaker University Teaching Hospital, Sfax, Tunisia
Abstract:The aims of this study are to investigate the frequency of derivative chromosome 9 (der (9)) deletion in Tunisian patients with chronic myeloid leukemia (CML) and to assess the correlation between this deletion and the cytogenetic response for patients treated with hydroxyurea (HU) or imatinib (IM). Karyotype analysis of 336 patients with CML was performed with R-banding technique. Fluorescence in situ hybridization (FISH) was carried using home-brew probes 17L7 and 248J22 for detecting, respectively, adjacent 5??ABL and 3??BCR deletions on der(9). Cytogenetic study demonstrated typical t(9;22)(q34;q11) translocation in 89.6% and variant translocation in 10.4% of patients. Interphase FISH studies showed deletion of der(9) in 59 (17.6%) of the 336 patients, 23 (39%) of them had variant rearrangements. There are 19 patients with solely 5??ABL deletion and 40 with concomitant 5??ABL and 3??BCR deletions. Cytogenetic response was evaluated during 18?months with HU or IM therapy. Our results demonstrate that (a) 3??BCR deletion is associated with 5??ABL deletion in all patients with der(9) deletions, (b) the 5??ABL and 3??BCR deletions arise simultaneously with t(9;22), (c) deletions on der(9) chromosome were frequently encountered in older patients and in patients presenting variant rearrangements, (d) both 5??ABL and 3??BCR deletions were associated with cytogenetic response failure in patients treated with HU, however, patients treated with IM and carrying der(9) deletions presented better cytogenetic response.
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