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Differential Regulation of Hypoxia-induced CXCR4 Triggering During B-cell Development and Lymphomagenesis

Overview
Journal Cancer Res
Specialty Oncology
Date 2007 Sep 19
PMID 17875700
Citations 23
Authors
Erich Piovan
Valeria Tosello
Stefano Indraccolo
Massimo Masiero
Luca Persano
Giovanni Esposito
Rita Zamarchi
Maurilio Ponzoni
Luigi Chieco-Bianchi
Riccardo Dalla-Favera
Alberto Amadori
Affiliations
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Abstract

The chemokine receptor CXCR4 plays a central role in organ-specific homing and tumor spreading and is induced by hypoxia. B lymphocytes are exposed to low oxygen tensions during their development, but the influence of hypoxia on their physiology is poorly understood. Here, we show that hypoxia is associated with up-regulation of CXCR4 expression in human normal and malignant B cells, through both transcriptional and posttranslational mechanisms. However, a dichotomic functional response to CXCR4 triggering was observed: both peripheral B cells and lymphomas arising from mature B cells displayed increased responses to CXCR4 triggering under hypoxia, whereas germinal center (GC) B cells as well as GC-derived lymphomas showed CXCR4 receptor desensitization. This phenomenon was associated with differential modulation of key signal-transducing molecules, including mitogen-activated protein kinase phosphatase-1 and regulator of G protein signaling molecule-1. The unresponsiveness of GC-derived lymphomatous B cells to CXCR4 triggering under hypoxia may have implications for the development and pathogenesis of GC-derived lymphoid tumors.

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