Abstract

Unlimited access to calorie-dense, palatable food is a hallmark of Western societies and substantially contributes to the worldwide rise of metabolic disorders. In addition to promoting overconsumption, palatable diets dampen daily intake patterns, further augmenting metabolic disruption. We developed a paradigm to reveal differential timing in the regulation of food intake behavior in mice. While homeostatic intake peaks in the active phase, conditioned place preference and choice experiments show an increased sensitivity to overeating on palatable food during the rest phase. This hedonic appetite rhythm is driven by endogenous circadian clocks in dopaminergic neurons of the ventral tegmental area (VTA). Mice with disrupted clock function in the VTA lose their hedonic overconsumption rhythms without affecting homeostatic intake. These findings assign a functional role of VTA clocks in modulating palatable feeding behaviors and identify a potential therapeutic route to counteract hyperphagy in an obesogenic environment.

Highlights

  • Unlimited access to calorie-dense, palatable food is a hallmark of Western societies and substantially contributes to the worldwide rise of metabolic disorders

  • The increasing prevalence of obesity has been recognized by the World Health Organization (WHO) as one of today’s principal challenges of the health system

  • Recent studies in rodents and humans suggest that the amount, and the timing of caloric intake plays an important role for the obesogenic properties of food, indicating a role of the circadian clock in the regulation of appetite and energy homeostasis[7,13]

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Summary

Introduction

Unlimited access to calorie-dense, palatable food is a hallmark of Western societies and substantially contributes to the worldwide rise of metabolic disorders. While homeostatic intake peaks in the active phase, conditioned place preference and choice experiments show an increased sensitivity to overeating on palatable food during the rest phase. This hedonic appetite rhythm is driven by endogenous circadian clocks in dopaminergic neurons of the ventral tegmental area (VTA). Our experiments reveal a circadian vulnerability to palatable foods peaking in the rest phase, roughly anti-phasic to homeostatic intake rhythms This hedonic appetite rhythm is controlled by clocks located in dopaminergic neurons of the VTA

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