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Abstract
The hepatic circadian clock plays a key role in the daily regulation of glucose metabolism, but the precise molecular mechanisms that coordinate these two biological processes are not fully understood. In this study, we identify a novel connection between the regulation of RORγ by the clock machinery and the diurnal regulation of glucose metabolic networks. We demonstrate that particularly at daytime, mice deficient in RORγ exhibit improved insulin sensitivity and glucose tolerance due to reduced hepatic gluconeogenesis. This is associated with a reduced peak expression of several glucose metabolic genes critical in the control of gluconeogenesis and glycolysis. Genome-wide cistromic profiling, promoter and mutation analysis support the concept that RORγ regulates the transcription of several glucose metabolic genes directly by binding ROREs in their promoter regulatory region. Similar observations were made in liver-specific RORγ-deficient mice suggesting that the changes in glucose homeostasis were directly related to the loss of hepatic RORγ expression. Altogether, our study shows that RORγ regulates several glucose metabolic genes downstream of the hepatic clock and identifies a novel metabolic function for RORγ in the diurnal regulation of hepatic gluconeogenesis and insulin sensitivity. The inhibition of the activation of several metabolic gene promoters by an RORγ antagonist suggests that antagonists may provide a novel strategy in the management of metabolic diseases, including type 2 diabetes.
Highlights
Receptor c (RORc) constitutes with RORa and RORb, the retinoic acidrelated orphan receptor (ROR; NR1F1–3) subfamily of the nuclear receptors, which regulate transcription by binding as monomers to ROR-responsive elements (ROREs) in the regulatory region of target genes [1,2]
By using ubiquitous and liver-specific RORc-deficient mice as models, we demonstrate that hepatic RORc modulates daily insulin sensitivity and glucose tolerance by regulating hepatic gluconeogenesis
We provide evidence for a model in which RORc regulates the circadian expression of glucose metabolic genes in the liver downstream of the hepatic circadian clock, thereby enhancing gluconeogenesis and decreasing insulin sensitivity and glucose tolerance
Summary
RORc constitutes with RORa and RORb, the retinoic acidrelated orphan receptor (ROR; NR1F1–3) subfamily of the nuclear receptors, which regulate transcription by binding as monomers to ROR-responsive elements (ROREs) in the regulatory region of target genes [1,2]. In contrast to RORct, relatively little is known about the physiological functions of RORc1. In several peripheral tissues RORc1 exhibits a robust rhythmic pattern of expression with a peak at zeitgeber time (ZT) 16–20 that is directly regulated by the clock proteins, brain and muscle ARNTlike (Bmal1) and circadian locomotor output cycles kaput (Clock), and the Rev-Erb nuclear receptors [1,8,9,10,11,12,14,15]. Since recent studies indicated an association between the level of RORc expression and obesityassociated insulin resistance in mice and humans [20,21], these
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