Early reappearance of intraclonal proliferative subpopulations in ibrutinib-resistant chronic lymphocytic leukemia.
Federico PozzoGabriela ForestieriFilippo VitGiulia IannaErika TissinoTamara BittoloRobel PapottiAnnalisa GaglioLodovico Terzi di BergamoAgostino SteffanJerry PoleselPietro BulianRoberta LaureanaAgostino TafuriAnnalisa ChiarenzaFrancesco Di RaimondoJacopo OlivieriFrancesco ZajaLuca LaurentiMaria Ilaria Del PrincipeMassimiliano PostorinoGiovanni Del PoetaRiccardo BombenAntonella ZucchettoDavide RossiValter GatteiPublished in: Leukemia (2024)
The Bruton's tyrosine kinase (BTK) inhibitor ibrutinib represents an effective strategy for treatment of chronic lymphocytic leukemia (CLL), nevertheless about 30% of patients eventually undergo disease progression. Here we investigated by flow cytometry the long-term modulation of the CLL CXCR4 dim /CD5 bright proliferative fraction (PF), its correlation with therapeutic outcome and emergence of ibrutinib resistance. By longitudinal tracking, the PF, initially suppressed by ibrutinib, reappeared upon early disease progression, without association with lymphocyte count or serum beta-2-microglobulin. Somatic mutations of BTK/PLCG2, detected in 57% of progressing cases, were significantly enriched in PF with a 3-fold greater allele frequency than the non-PF fraction, suggesting a BTK/PLCG2-mutated reservoir resident within the proliferative compartments. PF increase was also present in BTK/PLCG2-unmutated cases at progression, indicating that PF evaluation could represent a marker of CLL progression under ibrutinib. Furthermore, we evidence different transcriptomic profiles of PF at progression in cases with or without BTK/PLCG2 mutations, suggestive of a reactivation of B-cell receptor signaling or the emergence of bypass signaling through MYC and/or Toll-Like-Receptor-9. Clinically, longitudinal monitoring of the CXCR4 dim /CD5 bright PF by flow cytometry may provide a simple tool helping to intercept CLL progression under ibrutinib therapy.
Keyphrases
- chronic lymphocytic leukemia
- tyrosine kinase
- flow cytometry
- toll like receptor
- epidermal growth factor receptor
- end stage renal disease
- chronic kidney disease
- ejection fraction
- newly diagnosed
- nuclear factor
- stem cells
- cross sectional
- mass spectrometry
- transcription factor
- dna methylation
- mesenchymal stem cells
- single cell
- single molecule
- genome wide