B-Myb and cyclin D1 mediate heat shock element dependent activation of the human HSP70 promoter

被引:0
|
作者
Hiroshi Kamano
Karl-Heinz Klempnauer
机构
[1] Hans-Spemann-Laboratory,
[2] Max-Planck-Institute for Immunobiology,undefined
[3] Health Service Center,undefined
[4] Kagawa University,undefined
来源
Oncogene | 1997年 / 14卷
关键词
B-Myb; heat shock element; HSP70 pro-moter; cyclin D1;
D O I
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学科分类号
摘要
Previous studies have shown that B-Myb, a conserved member of the Myb transcription factor family, is a potent activator of the promoter of the human HSP70 gene but does not activate promoters containing Myb binding sites. We have now investigated the transactivation properties of B-Myb in more detail. We here report that B-Myb activates the HSP70 promoter by a novel mechanism which involves the heat shock element (HSE). Deletion analysis of B-Myb shows that a specific domain in the center of B-Myb, but not the DNA-binding domain is required for HSE-dependent transactivation. We also show that deletion of the C-terminal domain of B-Myb does not affect HSE-dependent transactivation but allows the protein to activate a promoter containing Myb binding sites. This suggests that the ability to activate Myb binding site containing promoters is repressed in the context of full length B-Myb and that HSE dependent and Myb binding site dependent transactivation are distinct functions of B-Myb. Finally, we report that cyclin D1 like B-Myb strongly activates the HSP70 promoter via the HSE. HSE-dependent transactivation is a novel activity of cyclin D1 and appears to be independent of the phosphorylation of the Rb protein. Our results reveal an interesting and unexpected connection between HSE-dependent gene activation and proteins expressed during the G1/S-transition of the cell cycle.
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页码:1223 / 1229
页数:6
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