| Literature DB >> 31786059 |
Rigo Cintron-Colon1, Christopher W Johnson2, J Rafael Montenegro-Burke3, Carlos Guijas3, Lila Faulhaber4, Manuel Sanchez-Alavez5, Carlos A Aguirre1, Kokila Shankar1, Mona Singh1, Andrea Galmozzi1, Gary Siuzdak6, Enrique Saez1, Bruno Conti7.
Abstract
Mammals maintain a nearly constant core body temperature (Tb) by balancing heat production and heat dissipation. This comes at a high metabolic cost that is sustainable if adequate calorie intake is maintained. When nutrients are scarce or experimentally reduced such as during calorie restriction (CR), endotherms can reduce energy expenditure by lowering Tb [1-6]. This adaptive response conserves energy, limiting the loss of body weight due to low calorie intake [7-10]. Here we show that this response is regulated by the kappa opioid receptor (KOR). CR is associated with increased hypothalamic levels of the endogenous opioid Leu-enkephalin, which is derived from the KOR agonist precursor dynorphin [11]. Pharmacological inhibition of KOR, but not of the delta or the mu opioid receptor subtypes, fully blocked CR-induced hypothermia and increased weight loss during CR independent of calorie intake. Similar results were seen with DIO mice subjected to CR. In contrast, inhibiting KOR did not change Tb in animals fed ad libitum (AL). Chemogenetic inhibition of KOR neurons in the hypothalamic preoptic area reduced the CR-induced hypothermia, whereas chemogenetic activation of prodynorphin-expressing neurons in the arcuate or the parabrachial nucleus lowered Tb. These data indicate that KOR signaling is a pivotal regulator of energy homeostasis and can affect body weight during dieting by modulating Tb and energy expenditure.Entities:
Keywords: body temperature; body weight; calorie restriction; dieting; dynorphin; energy expenditure; energy homeostasis; hypothermia; kappa opioid receptor
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Year: 2019 PMID: 31786059 PMCID: PMC6917995 DOI: 10.1016/j.cub.2019.10.027
Source DB: PubMed Journal: Curr Biol ISSN: 0960-9822 Impact factor: 10.834