Abstract
BCR-ABL is an aberrant tyrosine kinase responsible for chronic myeloid leukemia (CML). Tyrosine kinase inhibitors (TKIs) induce a potent antileukemic response mostly based on the inhibition of BCR-ABL, but they also increase the activity of Natural Killer (NK) and CD8+ T cells. After several years, patients may interrupt treatment due to sustained, deep molecular response. By unknown reasons, half of the patients relapse during treatment interruption, whereas others maintain a potent control of the residual leukemic cells for several years. In this study, several immunological parameters related to sustained antileukemic control were analyzed. According to our results, the features more related to poor antileukemic control were as follows: low levels of cytotoxic cells such as NK, (Natural Killer T) NKT and CD8±TCRγβ+ T cells; low expression of activating receptors on the surface of NK and NKT cells; impaired synthesis of proinflammatory cytokines or proteases from NK cells; and HLA-E*0103 homozygosis and KIR haplotype BX. A Random Forest algorithm predicted 90% of the accuracy for the classification of CML patients in groups of relapse or non-relapse according to these parameters. Consequently, these features may be useful as biomarkers predictive of CML relapse in patients that are candidates to initiate treatment discontinuation.
Highlights
Lorena Vigón 1, Alejandro Luna 2, Miguel Galán 3, Sara Rodríguez-Mora 1, Daniel Fuertes 4, Elena Mateos 1, Miguel Piris-Villaespesa 2, Guiomar Bautista 5, Esther San José 3, José Rivera-Torres 3, Juan Luis Steegmann 6, Fernando de Ory 7, Mayte Pérez-Olmeda 7, José Alcamí 1, Vicente Planelles 8, María Rosa López-Huertas 1, Valentín García-Gutiérrez 2, * and Mayte Coiras 1, *
Forty-five chronic myeloid leukemia (CML) patients were on treatment with Tyrosine kinase inhibitors (TKIs) (On TKI; dasatinib n = 18 (40%); imatinib n = 11 (24.4%); nilotinib n = 9 (20%); bosutinib n = 4 (8.9%); ponatinib n = 1 (2.3%); asciminib n = 2 (4.4%))
We evaluated the functionality of Natural Killer (NK) and NKT cell populations by measuring had CD3-CD56 + CD16+ NK cells in peripheral blood with high capacity to synthesize the synthesis of IFNγ, TNFα and granzyme B (GZB) in response to
Summary
Lorena Vigón 1 , Alejandro Luna 2 , Miguel Galán 3 , Sara Rodríguez-Mora 1 , Daniel Fuertes 4 , Elena Mateos 1 , Miguel Piris-Villaespesa 2 , Guiomar Bautista 5 , Esther San José 3 , José Rivera-Torres 3 , Juan Luis Steegmann 6 , Fernando de Ory 7 , Mayte Pérez-Olmeda 7 , José Alcamí 1 , Vicente Planelles 8 , María Rosa López-Huertas 1 , Valentín García-Gutiérrez 2, * and Mayte Coiras 1, *. Pharmacy and Biotechnology Department, Faculty of Biomedical Sciences, Universidad Europea de Madrid, School of Telecommunications Engineering, Universidad Politécnica de Madrid, 28040 Madrid, Spain; Hematology Service, Hospital Universitario Puerta de Hierro, 28222 Madrid, Spain; Serology Service, National Center of Microbiology, Instituto de Salud Carlos III, 28220 Madrid, Spain; Division of Microbiology and Immunology, University of Utah School of Medicine,. G.; San José, E.; Rivera-Torres, J.; et al Identification of Immunological Parameters as Predictive Biomarkers of Relapse in Patients with Chronic Myeloid. Publisher’s Note: MDPI stays neutral with regard to jurisdictional claims in published maps and institutional affiliations
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