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Structural and Functional Analysis of the Human Nuclear Xenobiotic Receptor PXR in Complex with RXRα.

J Mol Biol.. 2013-04;  S0022-2836(13):00243 - X
Wallace BD, Betts L, Talmage G, Pollet RM, Holman NS, Redinbo MR. Departments of Chemistry, Biochemistry and Microbiology, University of North Carolina at Chapel Hill, 250 Bell Tower Drive, Chapel Hill, NC 27599, USA.
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摘要

The human nuclear xenobiotic receptor PXR recognizes a range of potentially harmful drugs and endobiotic chemicals but must complex with the nuclear receptor RXRα to control the expression of numerous drug metabolism genes. To date, the structural basis and functional consequences of this interaction have remained unclear. Here we present 2.8-Å-resolution crystal structures of the heterodimeric complex formed between the ligand-binding domains of human PXR and RXRα. These structures establish that PXR and RXRα form a heterotetramer unprecedented in the nuclear receptor family of ligand-regulated transcription factors. We further show that both PXR and RXRα bind to the transcription... More

关键词

LBD, ligand-binding domain; DBD, DNA-binding domain; PDB, Protein Data Bank; MBP, maltose-binding protein