The crystal structure of a heterodimer between the ligand-binding domains (LBDs) of the human RAR alpha bound to a selective antagonist and the constitutively active mouse RXR alpha F318A mutant shows that, pushed by a bulky extension of the ligand, RAR alpha helix H12 adopts an antagonist position. The unexpected presence of a fatty acid in the ligand-binding pocket of RXR alpha F318A is likely to account for its apparent constitutivity. Specific conformational changes suggest the structural basis of pure and partial antagonism. The RAR-RXR heterodimer interface is similar to that observed in most nuclear receptor (NR) homodimers. A correlative analysis of 3D structures and sequences provides a novel view on dimerization among members of the nuclear receptor superfamily.
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