Peptide Antagonists of the Human Estrogen Receptor

John D. Norris; Lisa A. Paige; Dale J. Christensen; Ching‐yi Chang; Maria R. Huacani; Daju Fan; Paul T. Hamilton; Dana M. Fowlkes; Donald P. McDonnell

doi:10.1126/science.285.5428.744

Peptide Antagonists of the Human Estrogen Receptor

John D. Norris(Duke Medical Center), Lisa A. Paige, Dale J. Christensen, Ching‐yi Chang(Duke Medical Center), Maria R. Huacani(Duke Medical Center), Daju Fan(Duke Medical Center), Paul T. Hamilton, Dana M. Fowlkes, Donald P. McDonnell(Duke Medical Center)

Science

July 30, 1999

10.1126/science.285.5428.744

Cited by 377

Abstract

Estrogen receptor alpha transcriptional activity is regulated by distinct conformational states that are the result of ligand binding. Phage display was used to identify peptides that interact specifically with either estradiol- or tamoxifen-activated estrogen receptor alpha. When these peptides were coexpressed with estrogen receptor alpha in cells, they functioned as ligand-specific antagonists, indicating that estradiol-agonist and tamoxifen-partial agonist activities do not occur by the same mechanism. The ability to regulate estrogen receptor alpha transcriptional activity by targeting sites outside of the ligand-binding pocket has implications for the development of estrogen receptor alpha antagonists for the treatment of tamoxifen-refractory breast cancers.

Related Papers

No related papers found

Powered by citation graph analysis