| Literature DB >> 32066866 |
Elena Crisà1,2,3, Austin G Kulasekararaj4, Vera Adema5,6, Esperanza Such7,8, Julie Schanz9, Detlef Haase9, Katayoon Shirneshan9, Steven Best10, Syed A Mian4,11, Aytug Kizilors10, José Cervera12, Nicholas Lea10, Dario Ferrero13,14, Ulrich Germing15, Barbara Hildebrandt16, Ana Belén Valencia Martínez17, Valeria Santini13,17, Guillermo F Sanz7,8,18, Francesc Solé5, Ghulam J Mufti4.
Abstract
Monosomy 7 [-7] and/or partial loss of chromosome 7 [del(7q)] are associated with poor and intermediate prognosis, respectively, in myelodysplastic syndromes (MDS), but somatic mutations may also play a key complementary role. We analyzed the impact on the outcomes of deep targeted mutational screening in 280 MDS patients with -7/del(7q) as isolated cytogenetic abnormality (86 with del(7q) and 194 with -7). Patients with del(7q) or -7 had similar demographic and disease-related characteristics. Somatic mutations were detected in 79% (93/117) of patients (82% in -7 and 73% in del(7q) group). Median number of mutations per patient was 2 (range 0-8). There was no difference in mutation frequency between the two groups. Patients harbouring ≥2 mutations had a worse outcome than patients with <2 or no mutations (leukaemic transformation at 24 months, 38% and 20%, respectively, p = 0.044). Untreated patients with del(7q) had better overall survival (OS) compared with -7 (median OS, 34 vs 17 months, p = 0.034). In multivariable analysis, blast count, TP53 mutations and number of mutations were independent predictors of OS, whereas the cytogenetic subgroups did not retain prognostic relevance. This study highlights the importance of mutational analysis in terms of prognosis in MDS patients with isolated -7 or del(7q).Entities:
Mesh:
Year: 2020 PMID: 32066866 DOI: 10.1038/s41375-020-0728-x
Source DB: PubMed Journal: Leukemia ISSN: 0887-6924 Impact factor: 11.528