Altered neutrophil immunophenotypes in childhood B‐cell precursor acute lymphoblastic leukemia
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Publisher
Oncotarget
Abstract
An increasing number of evidences suggest a genetic predisposition in acute
lymphoblastic leukemia (ALL) that might favor the occurrence of the driver genetic
alterations. Such genetic background might also translate into phenotypic alterations
of residual hematopoietic cells. Whether such phenotypic alterations are present in
bone marrow (BM) cells from childhood B‑cell precursor (BCP)‑ALL remains to be
investigated. Here we analyzed the immunophenotypic profile of BM and peripheral
blood (PB) maturing/matured neutrophils from 118 children with BCP‑ALL and their
relationship with the features of the disease. Our results showed altered neutrophil
phenotypes in most (77%) BCP‑ALL cases. The most frequently altered marker
was CD10 (53%), followed by CD33 (34%), CD13 (15%), CD15/CD65 (10%) and
CD123 (7%). Of note, patients with altered neutrophil phenotypes had younger age
(p = 0.03) and lower percentages of BM maturing neutrophils (p = 0.004) together
with greater BM lymphocyte (p = 0.04), and mature B‑cell (p = 0.03) counts. No
significant association was found between an altered neutrophil phenotype and
other disease features. These findings point out the potential existence of an altered
residual hematopoiesis in most childhood BCP‑ALL cases.
Description
p. 24664-24676.: il. p&b. e color.
Keywords
Leucemia-Linfoma Linfoblástico de Células Precursoras, Precursor Cell Lymphoblastic Leukemia-Lymphoma, residual hematopoiesis,, Neutrófilos, Neutrophils, Imunofenotipagem, Immunophenotyping, Hematopoese, Hematopoiesis, Neoplasia Residual, Neoplasm Residual, Citometria de Fluxo, Flow Cytometry, Alarmes Clínicos, Clinical Alarms, Criança, Child
Citation
OLIVEIRA, Elen et al. Altered neutrophil immunophenotypes in childhood B‐cell precursor acute lymphoblastic leucemia. Oncotarget, n. 7, v. 17, p. 24664-24676, apr. 2016.