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Unravelling a clinical role of peripheral blood leukemia stem cells at diagnosis in chronic myeloid leukemia patients: Final results of prospective FLOWERS study

Academic Article
Publication Date:
2025
Short description:
Unravelling a clinical role of peripheral blood leukemia stem cells at diagnosis in chronic myeloid leukemia patients: Final results of prospective FLOWERS study / Sicuranza, Anna; Pacelli, Paola; Santoni, Adele; Abruzzese, Elisabetta; Cattaneo, Daniele; Iurlo, Alessandra; Luciano, Luigiana; Galimberti, Sara; Giai, Valentina; Mulas, Olga; Caocci, Giovanni; Sorà, Federica; Capodanno, Isabella; Crugnola, Monica; Gozzini, Antonella; Russo, Sabina; Annunziata, Mario; Fozza, Claudio; Cartocci, Alessandra; Fredducci, Sara; Pacini, Emanuele; Liberati, Anna Marina; Defina, Marzia; Bestoso, Elena; Marzano, Cristina; Tocci, Dania; Miracapillo, Teresa; Turriziani, Camilla; Peccia, Katia; Raspadori, Donatella; Bocchia, Monica. - In: CANCER. - ISSN 1097-0142. - 131:20(2025). [10.1002/cncr.70122]
abstract:
Background: The authors previously demonstrated that in peripheral blood (PB) of chronic myeloid leukemia (CML), patients’ leukemia stem cells (LSCs) CD26+ are detectable by flow cytometry at diagnosis, during tyrosine kinase inhibitor (TKI) therapy, and during treatment-free remission. Methods: This study presents results of a prospective multicenter study including 242 newly diagnosed CML patients monitored for PB CD26+ leukemic stem cells (LSCs) quantification from diagnosis up to 24 months of TKI treatment. Results: The bulk of CD26+ LSCs at diagnosis varied between patients with a median value of 7.14 cells/µL. During TKI treatment, it has been observed their consistent and rapid reduction without statistical differences according to type of first-line TKI. Instead, a significant correlation between a low amount of CD26+ LSCs at diagnosis and an optimal molecular response at 3, 12, and 24 months was documented (p =.03, p =.004, and p =.009, respectively). Three tertiles of CD26+ LSCs correlating to molecular response were identified: <3.21 cells/µL; between 3.21 and 19.21 cells/µL; and >19.21 cells/µL. The incidence of patients with optimal response was higher in the first CD26+ LSCs tertile respect to the third one (p =.027, p =.015, and p =.079, respectively) at all time points (3, 12 and 24 months). Conclusions: This study demonstrated a correlation between the amount of CD26+ LSCs at diagnosis and the molecular response, suggesting that the number of CD26+ LSCs at diagnosis could represent an additional tool for predicting TKI response.
Iris type:
1.1 Articolo in rivista
Keywords:
CD26; chronic myeloid leukemia; flow cytometry; leukemia stem cells; tyrosine kinase inhibitors
List of contributors:
Sicuranza, Anna; Pacelli, Paola; Santoni, Adele; Abruzzese, Elisabetta; Cattaneo, Daniele; Iurlo, Alessandra; Luciano, Luigiana; Galimberti, Sara; Giai, Valentina; Mulas, Olga; Caocci, Giovanni; Sorà, Federica; Capodanno, Isabella; Crugnola, Monica; Gozzini, Antonella; Russo, Sabina; Annunziata, Mario; Fozza, Claudio; Cartocci, Alessandra; Fredducci, Sara; Pacini, Emanuele; Liberati, Anna Marina; Defina, Marzia; Bestoso, Elena; Marzano, Cristina; Tocci, Dania; Miracapillo, Teresa; Turriziani, Camilla; Peccia, Katia; Raspadori, Donatella; Bocchia, Monica
Authors of the University:
FOZZA Claudio
Handle:
https://iris.uniss.it/handle/11388/372373
Published in:
CANCER
Journal
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