Regulation of circadian behaviour and metabolism by REV-ERB-α and REV-ERB-β

The nuclear receptors REV-ERB-α and REV-ERB-β are indispensible for the coordination of circadian rhythm and metabolism; mice without these nuclear receptors show disrupted circadian expression of core circadian clock and lipid homeostatic gene networks. Adjusting the metabolic clock Metabolic proce...

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Published in:Nature (London) 2012-05, Vol.485 (7396), p.123-127
Main Authors: Cho, Han, Zhao, Xuan, Hatori, Megumi, Yu, Ruth T., Barish, Grant D., Lam, Michael T., Chong, Ling-Wa, DiTacchio, Luciano, Atkins, Annette R., Glass, Christopher K., Liddle, Christopher, Auwerx, Johan, Downes, Michael, Panda, Satchidananda, Evans, Ronald M.
Format: Article
Language:English
Subjects:
631/337/2019
631/378/1385/2640
631/378/2583
631/443/376
Animals
Biological and medical sciences
Biological Clocks - drug effects
Biological Clocks - genetics
Circadian Rhythm - genetics
Circadian Rhythm - physiology
Circadian rhythms
Cryptochromes - deficiency
Cryptochromes - genetics
Cryptochromes - metabolism
Diverse techniques
Energy Metabolism - genetics
Feedback, Physiological
Fundamental and applied biological sciences. Psychology
Gene expression
Gene Expression Regulation
Gene Regulatory Networks - genetics
Genetic aspects
Genomes
Homeostasis - genetics
Humanities and Social Sciences
letter
Lipid Metabolism - genetics
Liver - metabolism
Male
Metabolism
Mice
Mice, Inbred C57BL
Mice, Knockout
Molecular and cellular biology
Molecular genetics
Molecular Sequence Data
Motor Activity - genetics
Motor Activity - physiology
multidisciplinary
Nuclear Receptor Subfamily 1, Group D, Member 1 - deficiency
Nuclear Receptor Subfamily 1, Group D, Member 1 - genetics
Nuclear Receptor Subfamily 1, Group D, Member 1 - metabolism
Period Circadian Proteins - deficiency
Period Circadian Proteins - genetics
Period Circadian Proteins - metabolism
Physiological aspects
Receptors, Cytoplasmic and Nuclear - deficiency
Receptors, Cytoplasmic and Nuclear - genetics
Receptors, Cytoplasmic and Nuclear - metabolism
Repressor Proteins - deficiency
Repressor Proteins - genetics
Repressor Proteins - metabolism
Science
Science (multidisciplinary)
Transcription. Transcription factor. Splicing. Rna processing
Transcriptome - genetics
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Summary:The nuclear receptors REV-ERB-α and REV-ERB-β are indispensible for the coordination of circadian rhythm and metabolism; mice without these nuclear receptors show disrupted circadian expression of core circadian clock and lipid homeostatic gene networks. Adjusting the metabolic clock Metabolic processes need to run like clockwork to prevent disease. Core clock proteins drive these rhythms, and the nuclear receptors REV-ERB-α and REV-ERB-β have a central role in regulating the expression of clock genes. Solt et al . report the identification of potent synthetic REV-ERB agonists, termed SR9011 and SR9009, which can alter the circadian expression of core clock genes in the hypothalami of mice. This is shown to alter the expression of metabolic genes in liver, skeletal-muscle and adipose tissue, and results in increased energy expenditure by the mice. The REV-ERB agonists reduce fat mass in diet-induced obese mice and improve dyslipidaemia and hyperglycaemia. These results suggest that synthetic REV-ERB ligands are promising candidates for the treatment of metabolic diseases. Cho et al . present genetic evidence that REV-ERB-α and REV-ERB-β are indispensible for the coordination of circadian rhythm and metabolism. Mice without REV-ERBs show disrupted expression of clock and lipid homeostatic gene networks. They have altered circadian wheel-running behaviour and deregulated lipid metabolism. These data ally REV-ERB-α and REV-ERB-β with PER, CRY and other components of the principal feedback loop that drives circadian expression. The circadian clock acts at the genomic level to coordinate internal behavioural and physiological rhythms via the CLOCK–BMAL1 transcriptional heterodimer. Although the nuclear receptors REV-ERB-α and REV-ERB-β have been proposed to form an accessory feedback loop that contributes to clock function 1 , 2 , their precise roles and importance remain unresolved. To establish their regulatory potential, we determined the genome-wide cis -acting targets (cistromes) of both REV-ERB isoforms in murine liver, which revealed shared recognition at over 50% of their total DNA binding sites and extensive overlap with the master circadian regulator BMAL1. Although REV-ERB-α has been shown to regulate Bmal1 expression directly 1 , 2 , our cistromic analysis reveals a more profound connection between BMAL1 and the REV-ERB-α and REV-ERB-β genomic regulatory circuits than was previously suspected. Genes within the intersection of the BMAL1, REV-ERB-α an
ISSN:0028-0836
1476-4687
DOI:10.1038/nature11048