JunB negatively regulates AP-1 activity and cell proliferation of malignant mouse keratinocytes

被引:0
|
作者
J. Finch
E. Joseloff
G. Bowden
机构
[1] Department of Radiation Oncology,
[2] University of Arizona,undefined
[3] Health Sciences Center,undefined
[4] Rm. 4993,undefined
[5] Arizona Cancer Center,undefined
[6] 1515 N. Campbell,undefined
[7] Tucson,undefined
[8] Ariz. 85724,undefined
[9] Celera Genomics,undefined
[10] 45 W. Gude Dr.,undefined
[11] Rockville,undefined
[12] MD 20850,undefined
关键词
Squamous cell carcinoma Cell proliferation AP-1 transactivation;
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摘要
Objective: Previously we have shown that a malignant mouse keratinocyte cell line, 10Gy5, has elevated AP-1 transactivation and reduced JunB protein levels compared to its parental benign cell line, 308, and that the tumorigenicity in the 10Gy5 cells could be blocked by a dominant negative c-Jun mutant protein. We wished to determine whether the change in JunB protein levels could account for the elevated AP-1 activity and whether re-expression of JunB in malignant 10Gy5 cells altered their proliferative capacity. Design: In the current study, we reduced JunB expression in benign 308 cells with antisense oligonucleotides and increased JunB expression in malignant 10Gy5 cells by stable transfection of a JunB expression vector. Results: Increased AP-1 activity was detected after treatment of the benign 308 cell line with JunB antisense oligonucleotides that reduced JunB protein levels. Stably JunB-transfected clones of malignant 10Gy5 cells showed decreased AP-1 activity, slowed in vitro cell proliferation and reduced tumor growth when xenografted to athymic nude mice. Conclusion: These findings suggest that expression of JunB protein has a negative effect on malignant tumor cell proliferation in part through its ability to inhibit AP-1 transactivation.
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页码:3 / 10
页数:7
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