We have determined the three-dimensional structures of both α- and β-forms of the ligand-binding domain of the oestrogen receptor (ER) in complexes with a range of receptor agonists and antagonists. Here, we summarize how these structures provide both an understanding of the ER's distinctive pharmacophore and a rationale for its ability to bind a diverse range of chemically distinct compounds. In addition, these studies provide a unique insight into the mechanisms that underlie receptor activation, as well as providing a structural basis for the antagonist action of molecules, such as raloxifene.

Keywords:
activation function 2, ligand binding, steroid receptor, transcription factor, AF1, activation function I, AF2, activation function 2, ER, oestrogen receptor, E2, 17-β-oestradiol, LBD, ligand-binding domain, NR, nuclear receptor
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© 2000 Biochemical Society
2000
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