Photoperiod modulates mu-opioid receptor availability in brown adipose tissue

Author:

Sun LihuaORCID,Aarnio Richard,Herre Erika Atencio,Kärnä Salli,Palani Senthil,Virtanen Helena,Liljenbäck Heidi,Virta Jenni,Honkaniemi Aake,Oikonen Vesa,Han Chunlei,Laurila SannaORCID,Bucci MarcoORCID,Helin Semi,Yatkin EmrahORCID,Nummenmaa LauriORCID,Nuutila PirjoORCID,Tang Jing,Roivainen Anne

Abstract

AbstractPhotoperiod drives metabolic activity of brown adipose tissue (BAT), and affects food intake and weight gain in mammals. Sympathetic innervation in BAT controls thermogenesis and facilitates physiological adaption to seasons, but the exact mechanism remains elusive. Previous studies show that the central opioid signaling tunes BAT heating and the brain muopioid receptor (MOR) levels have seasonal patterns. It is hence intriguing to know whether the peripheral MOR signaling shows seasonal variation. Here, we examined the effect of photoperiod on BAT MOR availability using [11C]carfentanil positron emission topography (PET). Adult rats (n = 9) were repeatedly imaged under changing photoperiods which simulates the local seasons. Long photoperiod downregulated MOR availability in BAT, while MOR availability in the muscles was unaffected. We confirmed the expression of MOR in BAT and muscle using immunofluorescence imaging. We conclude that photoperiod causally affects MOR availability in BAT, and sympathetic innervation of BAT may influence thermogenesis via the peripheral MOR system.Significance of the studyPhotoperiod impacts the metabolic activity of brown adipose tissue (BAT) with the exact mechanism still unclear. The current study shows that photoperiod causally affects the mu-opioid receptor (MOR) levels in BAT, with longer photoperiod leading to lower MOR availability. This possibly indicates down-regulated innervation during bright seasons. Immunofluorescence staining data reveal expression of MOR in both brain and peripheral tissues, drawing attention to the under-investigated peripheral MOR system. Also, the study highlights the feasibility of [11C]carfentanil PET in studying the peripheral MOR signaling.

Publisher

Cold Spring Harbor Laboratory

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