Transcription factors and breast cancer

doi:10.1677/erc.0.0050271

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Endocrine-Related Cancer 5 (4) 271-282 DOI: 10.1677/erc.0.0050271
Copyright © 1998 by the Society for Endocrinology.

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Transcription factors and breast cancer

C C Benz ¹

¹ Department of Medicine, University of California at San Francisco, California 94143, USA

Transcription factors are gene regulatory proteins endowedwith sequence-specific DNA recognition and the ability to positivelyor negatively influence the rate and efficiency of transcriptinitiation at a gene containing the factor's cognate recognition sequence,or DNA response element. Since transcription factors lie atthe heart of almost every fundamental developmental and homeostaticorganismal process- including DNA replication and repair, cellgrowth and division, control of apoptosis and cellular differentiation-it is not surprising that inherited or acquired defects in transcriptionfactor structure and function contribute to human carcinogenesis.As of 6 years ago a comprehensive list included greater than150 well characterized vertebrate transcription factors (Faisstand Meyer; 1992); individual families of transcription factorssuch as the Ets family, composed of only a few known membersat that time, have since grown to include greater than 30 members(Wasylyk and Nordheim; 1997). Furthermore, many of these samegene stimulating or repressing factors have been shown to haveoncogenic properties when genomically altered (mutated, rearranged,amplified or deleted), transcriptionally upregulated, or post-translationallymodified. Thus, we have come to realize that this growing bodyof transcription factors and the development-specific and tissue-restrictedgene programs under their control represent a rich and diversesource of mechanisms which, if disrupted, can lead to varioustypes of malignancy including breast cancer.

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Acknowledgements

This review is dedicated to the memory of Dr Helene Smith - a rigorous scientist, compassionate leader, and tireless champion of new ideas and efforts to understand and conquer breast cancer. This work was supported in part by NIH sponsored grants P01-CA44768, R01-CA36773, and R01-CA-71468 as well as the Hazel P Munroe and Janet Landfear memorial funds.