Abstract

Altered daily patterns of hormone action are suspected to contribute to metabolic disease. It is poorly understood how the adrenal glucocorticoid hormones contribute to the coordination of daily global patterns of transcription and metabolism. Here, we examined diurnal metabolite and transcriptome patterns in a zebrafish glucocorticoid deficiency model by RNA-Seq, NMR spectroscopy and liquid chromatography-based methods. We observed dysregulation of metabolic pathways including glutaminolysis, the citrate and urea cycles and glyoxylate detoxification. Constant, non-rhythmic glucocorticoid treatment rescued many of these changes, with some notable exceptions among the amino acid related pathways. Surprisingly, the non-rhythmic glucocorticoid treatment rescued almost half of the entire dysregulated diurnal transcriptome patterns. A combination of E-box and glucocorticoid response elements is enriched in the rescued genes. This simple enhancer element combination is sufficient to drive rhythmic circadian reporter gene expression under non-rhythmic glucocorticoid exposure, revealing a permissive function for the hormones in glucocorticoid-dependent circadian transcription. Our work highlights metabolic pathways potentially contributing to morbidity in patients with glucocorticoid deficiency, even under glucocorticoid replacement therapy. Moreover, we provide mechanistic insight into the interaction between the circadian clock and glucocorticoids in the transcriptional regulation of metabolism.

Highlights

  • The circadian clock is an endogenous oscillator that regulates daily changes of behavior, physiology and metabolism [1]

  • Production and release of glucocorticoids show a diurnal pattern regulated by the circadian clock

  • Altered daily patterns of hormone action are thought to contribute to metabolic diseases

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Summary

Introduction

The circadian clock is an endogenous oscillator that regulates daily changes of behavior, physiology and metabolism [1]. “peripheral” clocks in almost all tissues interact with signals produced by a “central” pacemaker, the hypothalamic suprachiasmatic nucleus. Hormones with metabolic functions are regulated by the circadian clock. This includes glucocorticoids (GCs), steroid hormones mainly produced by the adrenal gland [4]. GCs were shown to interact with clock factors in the transcriptional regulation of metabolic gene expression [5]. The global role of the interaction between the circadian clock and GCs in the regulation of physiology and metabolism and its underlying mechanisms are only incompletely understood

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