High levels of phosphorylated c-Jun, Fra-1, Fra-2 and ATF-2 proteins correlate with malignant phenotypes in the multistage mouse skin carcinogenesis model

被引:0
|
作者
Vassilis Zoumpourlis
Paraskevi Papassava
Spyros Linardopoulos
David Gillespie
Allan Balmain
Alexandros Pintzas
机构
[1] Institute of Biological Research and Biotechnology,
[2] National Hellenic Research Foundation,undefined
[3] Onyx Pharmaceuticals,undefined
[4] 3031 Research Drive,undefined
[5] CRC Beatson Laboratories,undefined
[6] Garscube Estate,undefined
[7] UCSF Cancer Center,undefined
来源
Oncogene | 2000年 / 19卷
关键词
ATF-2; mouse skin; AP-1; carcinogenesis;
D O I
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学科分类号
摘要
Analysis of the functions of AP-1 transcription factor in cellular systems has shown its key role as a mediator of oncogenic signals. The employment of suitable animal model systems greatly facilitates the study of changes in the composition and activity of the AP-1 complex. Here, we have analysed the quantitative and qualitative changes of AP-1 at different stages of carcinogenesis in mouse skin cell lines, derived from tumours induced by chemical mutagens. The findings of this study suggest that elevated AP-1 DNA binding and transactivation activity characterize the carcinoma cell lines, most notably the highly malignant spindle carcinomas. In addition, increased amounts and post-translational modifications of c-Jun, Fra-1, Fra-2 and ATF-2 proteins account for a high percentage of the increased AP-1 activity. Remarkably, high levels of phosphorylated ATF-2 protein were detected in malignant cell lines, indicating a novel role of ATF-2 in tumour progression. c-Jun and ATF-2 proteins are phosphorylated by highly active JNK kinases present in tumour cells. Finally, our results indicate distinct functions for different AP-1 components in the promotion and progression of mouse skin tumours.
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页码:4011 / 4021
页数:10
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