1. Ptp1b deletion in pro-opiomelanocortin neurons increases energy expenditure and impairs endothelial function via TNF-α dependent mechanisms
- Author
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Kendra K. Bence, Thiago Bruder-Nascimento, Galina Antonova, Eric J. Belin de Chantemèle, Simone Kennard, and James D. Mintz
- Subjects
0301 basic medicine ,endocrine system ,medicine.medical_specialty ,Pro-Opiomelanocortin ,Endothelium ,Adipose tissue ,Mice, Transgenic ,Arginine ,Weight Gain ,Superoxide dismutase ,03 medical and health sciences ,Internal medicine ,medicine ,Animals ,Obesity ,Endothelial dysfunction ,Neurons ,Protein Tyrosine Phosphatase, Non-Receptor Type 1 ,NADPH oxidase ,biology ,Tumor Necrosis Factor-alpha ,Leptin ,digestive, oral, and skin physiology ,Endothelial Cells ,General Medicine ,medicine.disease ,Nitric oxide synthase ,030104 developmental biology ,medicine.anatomical_structure ,Endocrinology ,Adipose Tissue ,Cyclooxygenase 2 ,biology.protein ,Tumor necrosis factor alpha ,Energy Metabolism ,hormones, hormone substitutes, and hormone antagonists - Abstract
Protein tyrosine phosphatase 1b (Ptp1b) is a negative regulator of leptin and insulin-signalling pathways. Its targeted deletion in proopiomelanocortin (POMC) neurons protects mice from obesity and diabetes by increasing energy expenditure. Inflammation accompanies increased energy expenditure. Therefore, the present study aimed to determine whether POMC-Ptp1b deletion increases energy expenditure via an inflammatory process, which would impair endothelial function. We characterized the metabolic and cardiovascular phenotypes of Ptp1b+/+ and POMC-Ptp1b−/− mice. Clamp studies revealed that POMC-Ptp1b deletion reduced body fat and increased energy expenditure as evidenced by a decrease in feed efficiency and an increase in oxygen consumption and respiratory exchange ratio. POMC-Ptp1b deletion induced a 2.5-fold increase in plasma tumour necrosis factor α (TNF-α) levels and elevated body temperature. Vascular studies revealed an endothelial dysfunction in POMC-Ptp1b−/− mice. Nitric oxide synthase inhibition [N-nitro-L-arginine methyl ester (L-NAME)] reduced relaxation to a similar extent in Ptp1b+/+ and POMC-Ptp1b−/− mice. POMC-Ptp1b deletion decreased ROS-scavenging enzymes [superoxide dismutases (SODs)] whereas it increased ROS-generating enzymes [NADPH oxidases (NOXs)] and cyclooxygenase-2 (COX-1) expression, in aorta. ROS scavenging or NADPH oxidase inhibition only partially improved relaxation whereas COX-2 inhibition and thromboxane-A2 (TXA2) antagonism fully restored relaxation in POMC-Ptp1b−/− mice. Chronic treatment with the soluble TNF-α receptor etanercept decreased body temperature, restored endothelial function and reestablished aortic COX-2, NOXs and SOD expression to their baseline levels in POMC-Ptp1b−/− mice. However, etanercept promoted body weight gain and decreased energy expenditure in POMC-Ptp1b−/− mice. POMC-Ptp1b deletion increases plasma TNF-α levels, which contribute to body weight regulation via increased energy expenditure and impair endothelial function via COX-2 and ROS-dependent mechanisms.
- Published
- 2016
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