Journal
CANCER RESEARCH
Volume 66, Issue 8, Pages 3978-3980Publisher
AMER ASSOC CANCER RESEARCH
DOI: 10.1158/0008-5472.CAN-05-4418
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Previous studies have shown that the interleukin-12 receptor beta 2 (IL-12R beta 2) gene is expressed in normal naive, germinal center and memory B cells but not in their malignant counterparts. The aim of this study was to investigate (i),whether the IL-12B beta 2 gene is silenced in B-cell acute lymphoblastic leukemia (B-ALL) cells, and (U) what the functional implications of such silencing for tumor growth are. Here, we show that although mature B cells expressed both chains of the IL-12R, normal pro-B and pre-B cells failed to express the IL-12R beta 2 chain. Similarly, primary tumor cells from pediatric pro-B, early pre-B, and pre-B ALL (30 cases) did not express the IL-12R beta 2 chain. IL-12R beta 2 gene silencing in WALL was found to depend on methylation of a CpG island in exon 1. Such methylation was not detected in normal early B cells that when differentiated into mature B cells expressed the IL-12R beta 2 gene. Detection of IL-12R beta 2 mRNA and protein in the tumorigenic 697 pre-B-ALL cell line allowed to perform functional experiments in severe combined immunodeficient/ nonobese diabetic mice receiving 697 cells with or without human recombinant IL-12 (hrIL-12). hrIL-12 administration reduced tumor growth and metastasis through antiproliferative and proapoptotic rather than antiangiogenic, activities. In conclusion, epigenetic silencing of the IL-12R beta 2 gene represents a novel mechanism of tumor escape for B-ALL cells.
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