High CXCR3 on Leukemic Cells Distinguishes [IgHV.sup.mut] from [IgHV.sup.unmut] in Chronic Lymphocytic Leukemia: Evidence from [CD5.sup.high] and [CD5.sup.low] Clones

High CXCR3 on Leukemic Cells Distinguishes [IgHV.sup.mut] from [IgHV.sup.unmut] in Chronic Lymphocytic Leukemia: Evidence from [CD5.sup.high] and [CD5.sup.low] Clones

Despite the shared pattern of surface antigens, neoplastic cells in chronic lymphocytic leukemia (CLL) are highly heterogeneous in CD5 expression, a marker linked to a proliferative pool of neoplastic cells. To further characterize [CD5.sup.high] and [CD5.sup.low] neoplastic cells, we assessed the c...

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Veröffentlicht in:Journal of Immunology Research 2020-06, Vol.2020
Hauptverfasser: Manukyan, Gayane, Papajik, Tomas, Mikulkova, Zuzana, Urbanova, Renata, Kraiczova, Veronika Smotkova, Savara, Jakub, Kudelka, Milos, Turcsanyi, Peter, Kriegova, Eva
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Analysis
B cells
Chronic lymphocytic leukemia
Cloning
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container_title Journal of Immunology Research
container_volume 2020
creator Manukyan, Gayane
Papajik, Tomas
Mikulkova, Zuzana
Urbanova, Renata
Kraiczova, Veronika Smotkova
Savara, Jakub
Kudelka, Milos
Turcsanyi, Peter
Kriegova, Eva
description Despite the shared pattern of surface antigens, neoplastic cells in chronic lymphocytic leukemia (CLL) are highly heterogeneous in CD5 expression, a marker linked to a proliferative pool of neoplastic cells. To further characterize [CD5.sup.high] and [CD5.sup.low] neoplastic cells, we assessed the chemokine receptors (CCR5, CCR7, CCR10, CXCR3, CXCR4, CXCR5) and adhesion molecules (CD54, CD62L, CD49d) on the [CD5.sup.high] and [CD5.sup.low] subpopulations, defined by CD5/CD19 coexpression, in peripheral blood of CLL patients (n = 60) subgrouped according to the IgHV mutational status ([IgHV.sup.mut], n = 24; [IgHVn.sup.mut], n = 36). [CD5.sup.high] subpopulation showed a high percentage of CXCR3 (P < 0.001), CCR10 (P = 0.001), and CD62L (P = 0.031) and high levels of CXCR5 (P = 0.005), CCR7 (P = 0.013) compared to [CD5.sup.low] cells expressing high CXCR4 (P < 0.001). Comparing [IgHV.sup.mut] and [IgHV.sup.unmut] patients, high levels of CXCR3 on [CD5.sup.high] and [CD5.sup.low] subpopulations were detected in the [IgHV.sup.mut] patients, with better discrimination in [CD5.sup.low] subpopulation. Levels of CXCR3 on [CD5.sup.low] subpopulation were associated with time to the next treatment, thus further confirming its prognostic value. Taken together, our analysis revealed higher CXCR3 expression on both [CD5.sup.high] and [CD5.sup.low] neoplastic cells in [IgHV.sup.mut] with a better prognosis compared to [IgHV.sup.unmut] patients. Contribution of CXCR3 to CLL pathophysiology and its suitability for prognostication and therapeutic exploitation deserves future investigations.
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To further characterize [CD5.sup.high] and [CD5.sup.low] neoplastic cells, we assessed the chemokine receptors (CCR5, CCR7, CCR10, CXCR3, CXCR4, CXCR5) and adhesion molecules (CD54, CD62L, CD49d) on the [CD5.sup.high] and [CD5.sup.low] subpopulations, defined by CD5/CD19 coexpression, in peripheral blood of CLL patients (n = 60) subgrouped according to the IgHV mutational status ([IgHV.sup.mut], n = 24; [IgHVn.sup.mut], n = 36). [CD5.sup.high] subpopulation showed a high percentage of CXCR3 (P &lt; 0.001), CCR10 (P = 0.001), and CD62L (P = 0.031) and high levels of CXCR5 (P = 0.005), CCR7 (P = 0.013) compared to [CD5.sup.low] cells expressing high CXCR4 (P &lt; 0.001). Comparing [IgHV.sup.mut] and [IgHV.sup.unmut] patients, high levels of CXCR3 on [CD5.sup.high] and [CD5.sup.low] subpopulations were detected in the [IgHV.sup.mut] patients, with better discrimination in [CD5.sup.low] subpopulation. Levels of CXCR3 on [CD5.sup.low] subpopulation were associated with time to the next treatment, thus further confirming its prognostic value. Taken together, our analysis revealed higher CXCR3 expression on both [CD5.sup.high] and [CD5.sup.low] neoplastic cells in [IgHV.sup.mut] with a better prognosis compared to [IgHV.sup.unmut] patients. 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To further characterize [CD5.sup.high] and [CD5.sup.low] neoplastic cells, we assessed the chemokine receptors (CCR5, CCR7, CCR10, CXCR3, CXCR4, CXCR5) and adhesion molecules (CD54, CD62L, CD49d) on the [CD5.sup.high] and [CD5.sup.low] subpopulations, defined by CD5/CD19 coexpression, in peripheral blood of CLL patients (n = 60) subgrouped according to the IgHV mutational status ([IgHV.sup.mut], n = 24; [IgHVn.sup.mut], n = 36). [CD5.sup.high] subpopulation showed a high percentage of CXCR3 (P &lt; 0.001), CCR10 (P = 0.001), and CD62L (P = 0.031) and high levels of CXCR5 (P = 0.005), CCR7 (P = 0.013) compared to [CD5.sup.low] cells expressing high CXCR4 (P &lt; 0.001). Comparing [IgHV.sup.mut] and [IgHV.sup.unmut] patients, high levels of CXCR3 on [CD5.sup.high] and [CD5.sup.low] subpopulations were detected in the [IgHV.sup.mut] patients, with better discrimination in [CD5.sup.low] subpopulation. Levels of CXCR3 on [CD5.sup.low] subpopulation were associated with time to the next treatment, thus further confirming its prognostic value. Taken together, our analysis revealed higher CXCR3 expression on both [CD5.sup.high] and [CD5.sup.low] neoplastic cells in [IgHV.sup.mut] with a better prognosis compared to [IgHV.sup.unmut] patients. 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To further characterize [CD5.sup.high] and [CD5.sup.low] neoplastic cells, we assessed the chemokine receptors (CCR5, CCR7, CCR10, CXCR3, CXCR4, CXCR5) and adhesion molecules (CD54, CD62L, CD49d) on the [CD5.sup.high] and [CD5.sup.low] subpopulations, defined by CD5/CD19 coexpression, in peripheral blood of CLL patients (n = 60) subgrouped according to the IgHV mutational status ([IgHV.sup.mut], n = 24; [IgHVn.sup.mut], n = 36). [CD5.sup.high] subpopulation showed a high percentage of CXCR3 (P &lt; 0.001), CCR10 (P = 0.001), and CD62L (P = 0.031) and high levels of CXCR5 (P = 0.005), CCR7 (P = 0.013) compared to [CD5.sup.low] cells expressing high CXCR4 (P &lt; 0.001). Comparing [IgHV.sup.mut] and [IgHV.sup.unmut] patients, high levels of CXCR3 on [CD5.sup.high] and [CD5.sup.low] subpopulations were detected in the [IgHV.sup.mut] patients, with better discrimination in [CD5.sup.low] subpopulation. Levels of CXCR3 on [CD5.sup.low] subpopulation were associated with time to the next treatment, thus further confirming its prognostic value. Taken together, our analysis revealed higher CXCR3 expression on both [CD5.sup.high] and [CD5.sup.low] neoplastic cells in [IgHV.sup.mut] with a better prognosis compared to [IgHV.sup.unmut] patients. Contribution of CXCR3 to CLL pathophysiology and its suitability for prognostication and therapeutic exploitation deserves future investigations.</abstract><pub>John Wiley &amp; Sons, Inc</pub></addata></record>
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subjects Analysis
B cells
Chronic lymphocytic leukemia
Cloning
title High CXCR3 on Leukemic Cells Distinguishes [IgHV.sup.mut] from [IgHV.sup.unmut] in Chronic Lymphocytic Leukemia: Evidence from [CD5.sup.high] and [CD5.sup.low] Clones
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