Regulation of circadian behaviour and metabolism by synthetic REV-ERB agonists

Solt, Laura A.; Wang, Yongjun; Banerjee, Subhashis; Hughes, Travis S.; Kojetin, D.J.; Lundåsen, Thomas; Shin, Youseung; Liu, Jin; Cameron, Michael D.; Noël, Romain; Yoo, Seung-Hee; Takahashi, Joseph S.; Butler, Andrew A.; Kamenecka, Theodore M.; Burris, Thomas P.

doi:10.1038/nature11030

Cited by 655 publications

(715 citation statements)

References 28 publications

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“…Rev-erb intervient aussi dans le développement du tissu adipeux et la synthèse des acides biliaires et du glucose [37]. Le traitement de souris avec des ligands synthétiques de Rev-erb/ induit une perte de poids et l'amélioration de la sensibilité à l'insuline [38]. ROR régule le méta-bolisme des lipides et la synthèse des acides biliaires parallèlement à son action sur Bmal1 [39].…”

Section: Couplage De L'horloge Moléculaire Avec Le Statut Métaboliqueunclassified

Horloges circadiennes et métabolisme : intégration des signaux métaboliques et environnementaux

2013

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Section: Couplage De L'horloge Moléculaire Avec Le Statut Métaboliqueunclassified

Horloges circadiennes et métabolisme : intégration des signaux métaboliques et environnementaux

2013

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“…deux gènes sont invalidés ont une stéa-tose hépatique sévère, sont hyperglycémiques et quasiment arythmiques, même en présence d'un cycle de lumière et d'obscurité [7][8][9] (➜). Nos résultats, ainsi que ces autres travaux, ouvrent la voie au développe-ment de nouvelles stratégies thérapeutiques ciblant les voies de signalisation associées aux protéines REVERB pour limiter ou traiter les désordres circadiens et leurs consé-quences sur l'homéostasie énergétique, comme l'illustre d'ailleurs une autre publication récente [10]. ◊ When our metabolic health depends on our internal clocks…”

Section: Les Protéines D'horlogeunclassified

Implications du gène d’horlogeReverbαdans l’obésité

2012

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“…Although heme has been identified as the ligand for Rev-erb-α [15,16], evidence suggests the Drosophila orthologue to Rev-erb-α binds CO and represses gene expression [10]. Whether or not the expression of Rev-erb-α targets is altered in tissues following CO treatment is not known, although a Rev-erb agonist has been shown to promote weight loss and suppress PGC-1α mRNA expression, an established target of Rev-erb-α [14].…”

Section: Introductionmentioning

confidence: 99%

“…Rev-erb-α is a ligand regulated transcription factor that acts as a transcriptional repressor [11,12] regulating circadian rhythms and metabolism [13,14]. Although heme has been identified as the ligand for Rev-erb-α [15,16], evidence suggests the Drosophila orthologue to Rev-erb-α binds CO and represses gene expression [10].…”

Section: Introductionmentioning

confidence: 99%

The effects of chronic carbon monoxide treatment on diet-induced obesity and Rev-erb-alpha target gene expression in adipose tissue

Brodsky¹,

McLoughlin²,

Sell³

et al. 2016

Integr Obesity Diabetes

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The present study determined if carbon monoxide (CO) treatment reversed diet-induced obesity and insulin resistance. Because CO is a potential ligand for the nuclear receptor Rev-erb-α, we also determined if CO treatment altered the mRNA expression of Rev-erb-α targets. Mice were fed a low fat diet (LFD) or a high fat diet (HFD) for 150 days. Following 110 days of the dietary intervention the HFD-fed mice were assigned to a CO inhalation group or a control group. The HFD-CO group was exposed to 250 ppm CO for one hour per day for 40 consecutive days. Body weight and edpididymal white adipose tissue (EWAT) mass were significantly elevated in HFD and HFD-CO mice compared to LFD mice, but no differences existed between HFD and HFD-CO mice. Area under the insulin-assisted glucose tolerance curve was significantly elevated in HFD and HFD-CO mice compared to LFD mice, but no differences existed between HFD and HFD-CO mice. Heme oxygenase-1 (HO-1) mRNA was significantly higher in EWAT of HFD-CO compared to HFD mice, indicating effective delivery of CO to adipose tissue. CO treatment did not alter Rev-erb-α expression or Rev-erb-α targets. These results indicate that CO inhalation does not attenuate diet-induced obesity/insulin resistance.

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Regulation of circadian behaviour and metabolism by synthetic REV-ERB agonists

Cited by 655 publications

References 28 publications

Horloges circadiennes et métabolisme : intégration des signaux métaboliques et environnementaux

Horloges circadiennes et métabolisme : intégration des signaux métaboliques et environnementaux

Implications du gène d’horlogeReverbαdans l’obésité

The effects of chronic carbon monoxide treatment on diet-induced obesity and Rev-erb-alpha target gene expression in adipose tissue

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