1err
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HUMAN ESTROGEN RECEPTOR LIGAND-BINDING DOMAIN IN COMPLEX WITH RALOXIFENE
OverviewOverview
Oestrogens are involved in the growth, development and homeostasis of a, number of tissues. The physiological effects of these steroids are, mediated by a ligand-inducible nuclear transcription factor, the oestrogen, receptor (ER). Hormone binding to the ligand-binding domain (LBD) of the, ER initiates a series of molecular events culminating in the activation or, repression of target genes. Transcriptional regulation arises from the, direct interaction of the ER with components of the cellular transcription, machinery. Here we report the crystal structures of the LBD of ER in, complex with the endogenous oestrogen, 17beta-oestradiol, and the, selective antagonist raloxifene, at resolutions of 3.1 and 2.6 A, respectively. The structures provide a molecular basis for the distinctive, pharmacophore of the ER and its catholic binding properties. Agonist and, antagonist bind at the same site within the core of the LBD but, demonstrate different binding modes. In addition, each class of ligand, induces a distinct conformation in the transactivation domain of the LBD, providing structural evidence of the mechanism of antagonism.
DiseaseDisease
Known diseases associated with this structure: Atherosclerosis, susceptibility to OMIM:[133430], Breast cancer OMIM:[133430], Estrogen resistance OMIM:[133430], HDL response to hormone replacement, augmented OMIM:[133430], Migraine, susceptibility to OMIM:[133430], Myocardial infarction, susceptibility to OMIM:[133430]
About this StructureAbout this Structure
1ERR is a Single protein structure of sequence from Homo sapiens with RAL as ligand. Full crystallographic information is available from OCA.
ReferenceReference
Molecular basis of agonism and antagonism in the oestrogen receptor., Brzozowski AM, Pike AC, Dauter Z, Hubbard RE, Bonn T, Engstrom O, Ohman L, Greene GL, Gustafsson JA, Carlquist M, Nature. 1997 Oct 16;389(6652):753-8. PMID:9338790
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