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Publication : Histone H2AX suppresses translocations in lymphomas of Eμ-c-Myc transgenic mice that contain a germline amplicon of tumor-promoting genes.

First Author  Fusello A Year  2013
Journal  Cell Cycle Volume  12
Issue  17 Pages  2867-75
PubMed ID  23966158 Mgi Jnum  J:317301
Mgi Id  MGI:6852288 Doi  10.4161/cc.25922
Citation  Fusello A, et al. (2013) Histone H2AX suppresses translocations in lymphomas of Emu-c-Myc transgenic mice that contain a germline amplicon of tumor-promoting genes. Cell Cycle 12(17):2867-75
abstractText  The DNA damage response (DDR) can restrain the ability of oncogenes to cause genomic instability and drive malignant transformation. The gene encoding the histone H2AX DDR factor maps to 11q23, a region frequently altered in human cancers. Since H2ax functions as a haploinsufficient suppressor of B lineage lymphomas with c-Myc amplification and/or translocation, we determined the impact of H2ax expression on the ability of deregulated c-Myc expression to cause genomic instability and drive transformation of B cells. Neither H2ax deficiency nor haploinsufficiency affected the rate of mortality of Emu-c-Myc mice from B lineage lymphomas with genomic deletions and amplifications. Yet H2ax functioned in a dosage-dependent manner to prevent unbalanced translocations in Emu-c-Myc tumors, demonstrating that H2ax functions in a haploinsufficient manner to suppress allelic imbalances and limit molecular heterogeneity within and among Emu-c-Myc lymphomas. Regardless of H2ax copy number, all Emu-c-Myc tumors contained identical amplification of chromosome 19 sequences spanning 20 genes. Many of these genes encode proteins with tumor-promoting activities, including Cd274, which encodes the PD-L1 programmed death ligand that induces T cell apoptosis and enables cancer cells to escape immune surveillance. This amplicon was in non-malignant B and T cells and non-lymphoid cells, linked to the Emu-c-Myc transgene, and associated with overexpression of PD-L1 on non-malignant B cells. Our data demonstrate that, in addition to deregulated c-Myc expression, non-malignant B lineage lymphocytes of Emu-c-Myc transgenic mice may have constitutive amplification and increased expression of other tumor-promoting genes.
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