Chronic Intermittent Hypoxia during Sleep Causes Browning of Interscapular Adipose Tissue Accompanied by Local Insulin Resistance in Mice.
Tehila DahanShahd NassarOlga YajukEliana SteinbergOfra BennyNathalie AbudiInbar PlaschkesHadar BenyaminiDavid GozalRinat AbramovitchAlex Gileles-HillelPublished in: International journal of molecular sciences (2022)
Obstructive sleep apnea (OSA) is a highly prevalent condition, characterized by intermittent hypoxia (IH), sleep disruption, and altered autonomic nervous system function. OSA has been independently associated with dyslipidemia, insulin resistance, and metabolic syndrome. Brown adipose tissue (BAT) has been suggested as a modulator of systemic glucose tolerance through adaptive thermogenesis. Reductions in BAT mass have been associated with obesity and metabolic syndrome. No studies have systematically characterized the effects of chronic IH on BAT. Thus, we aimed to delineate IH effects on BAT and concomitant metabolic changes. C57BL/6J 8-week-old male mice were randomly assigned to IH during sleep (alternating 90 s cycles of 6.5% F I O 2 followed by 21% F I O 2 ) or normoxia (room air, RA) for 10 weeks. Mice were subjected to glucose tolerance testing and 18 F-FDG PET-MRI towards the end of the exposures followed by BAT tissues analyses for morphological and global transcriptomic changes. Animals exposed to IH were glucose intolerant despite lower total body weight and adiposity. BAT tissues in IH-exposed mice demonstrated characteristic changes associated with "browning"-smaller lipids, increased vascularity, and a trend towards higher protein levels of UCP1. Conversely, mitochondrial DNA content and protein levels of respiratory chain complex III were reduced. Pro-inflammatory macrophages were more abundant in IH-exposed BAT. Transcriptomic analysis revealed increases in fatty acid oxidation and oxidative stress pathways in IH-exposed BAT, along with a reduction in pathways related to myogenesis, hypoxia, and IL-4 anti-inflammatory response. Functionally, IH-exposed BAT demonstrated reduced absorption of glucose on PET scans and reduced phosphorylation of AKT in response to insulin. Current studies provide initial evidence for the presence of a maladaptive response of interscapular BAT in response to chronic IH mimicking OSA, resulting in a paradoxical divergence, namely, BAT browning but tissue-specific and systemic insulin resistance. We postulate that oxidative stress, mitochondrial dysfunction, and inflammation may underlie these dichotomous outcomes in BAT.
Keyphrases
- insulin resistance
- high fat diet induced
- adipose tissue
- metabolic syndrome
- oxidative stress
- obstructive sleep apnea
- type diabetes
- mitochondrial dna
- high fat diet
- skeletal muscle
- computed tomography
- polycystic ovary syndrome
- body weight
- positron emission tomography
- positive airway pressure
- fatty acid
- clinical trial
- dna damage
- gene expression
- magnetic resonance imaging
- magnetic resonance
- blood pressure
- sleep quality
- glycemic control
- rheumatoid arthritis
- randomized controlled trial
- high intensity
- contrast enhanced
- small molecule
- cardiovascular disease
- uric acid
- nitric oxide
- heart rate
- drug induced
- wild type
- endoplasmic reticulum stress
- systemic sclerosis
- weight gain
- genome wide
- induced apoptosis
- interstitial lung disease
- placebo controlled
- sleep apnea