The Runx1 transcription factor controls CSF-1-dependent and -independent growth and survival of macrophages

被引:0
|
作者
Stewart R Himes
Stephen Cronau
Christine Mulford
David A Hume
机构
[1] CRC for Chronic Inflammatory Disease,
[2] Institute for Molecular Biosciences,undefined
[3] Queensland Biosciences Precinct,undefined
[4] Bldg. 80,undefined
[5] Services Rd.,undefined
[6] University of Queensland,undefined
来源
Oncogene | 2005年 / 24卷
关键词
Runx1; macrophage; CSF-1; survival;
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中图分类号
学科分类号
摘要
Gene translocations that repress the function of the Runx1 transcription factor play a critical role in the development of myeloid leukemia. In this report, we demonstrate that Runx1 precisely regulates c-fms (CSF-1 receptor) gene expression. Runx1 controlled expression by binding to multiple sites within the mouse c-fms gene, allowing interaction between promoter and downstream enhancer elements. The runx1 and c-fms genes showed an identical pattern of expression in mature macrophages. Runx1 expression was repressed in CSF-1 stimulated, proliferating bone marrow-derived macrophages (BMM) and significantly increased in quiescent, CSF-1 starved cells. The RAW264.7 and Mono-Mac-6, macrophage-like cell lines expressed low levels of Runx1 and both showed growth arrest and cell death with ectopic expression of Runx1. The EM-3 cell line, which represents an early myeloid progenitor cell line, showed growth arrest with Runx1 expression in the absence of any detectable changes in cell differentiation. These findings suggest that Runx1 regulates growth and survival of myeloid cells and provide a novel insight into the role of Runx family gene translocations in leukemogenesis.
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页码:5278 / 5286
页数:8
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