Literature DB >> 18037887

Identification of heme as the ligand for the orphan nuclear receptors REV-ERBalpha and REV-ERBbeta.

Srilatha Raghuram1, Keith R Stayrook, Pengxiang Huang, Pamela M Rogers, Amanda K Nosie, Don B McClure, Lorri L Burris, Sepideh Khorasanizadeh, Thomas P Burris, Fraydoon Rastinejad.   

Abstract

The nuclear receptors REV-ERBalpha (encoded by NR1D1) and REV-ERBbeta (NR1D2) have remained orphans owing to the lack of identified physiological ligands. Here we show that heme is a physiological ligand of both receptors. Heme associates with the ligand-binding domains of the REV-ERB receptors with a 1:1 stoichiometry and enhances the thermal stability of the proteins. Results from experiments of heme depletion in mammalian cells indicate that heme binding to REV-ERB causes the recruitment of the co-repressor NCoR, leading to repression of target genes including BMAL1 (official symbol ARNTL), an essential component of the circadian oscillator. Heme extends the known types of ligands used by the human nuclear receptor family beyond the endocrine hormones and dietary lipids described so far. Our results further indicate that heme regulation of REV-ERBs may link the control of metabolism and the mammalian clock.

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Year:  2007        PMID: 18037887      PMCID: PMC2743565          DOI: 10.1038/nsmb1344

Source DB:  PubMed          Journal:  Nat Struct Mol Biol        ISSN: 1545-9985            Impact factor:   15.369


  58 in total

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  258 in total

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8.  A small molecule modulates circadian rhythms through phosphorylation of the period protein.

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Review 9.  Structural and functional insights into nuclear receptor signaling.

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10.  Regulation of intracellular heme trafficking revealed by subcellular reporters.

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