Abstract

Several studies suggest a role of extracellular adenine nucleotides in regulating adipose tissue functions via the purinergic signaling network. Metabolic studies in mice with global deletion of the purinergic receptor P2X7 on the C57BL/6 background indicate that this receptor has only a minor role in adipose tissue for diet-induced inflammation or cold-triggered thermogenesis. However, recent data show that a polymorphism (P451L) present in C57BL/6 mice attenuates P2X7 receptor function, whereas BALB/c mice express the fully functional P451 allele. To determine the potential role of P2rx7 under metabolic and thermogenic stress conditions, we performed comparative studies using male P2rx7 knockout (KO) and respective wild-type controls on both BALB/c and C57BL/6 backgrounds. Our data show that adipose P2rx7 mRNA levels are increased in obese mice. Moreover, P2rx7 deficiency results in reduced levels of circulating CCL2 and IL6 with a moderate effect on gene expression of pro-inflammatory markers in white adipose tissue and liver of BALB/c and C57BL/6 mice. However, P2X7 expression does not alter body weight, insulin resistance, and hyperglycemia associated with high-fat diet feeding on both genetic backgrounds. Furthermore, deficiency of P2rx7 is dispensable for energy expenditure at thermoneutral and acute cold exposure conditions. In summary, these data show that—apart from a moderate effect on inflammatory cytokines—P2X7 plays only a minor role in inflammatory and thermogenic effects of white and brown adipose tissue even on the BALB/c background.

Highlights

  • Adipose tissue is a complex organ with an important role in endocrine, metabolic, and immune regulatory processes

  • To assess the effect of nutritional state on expression of enzymes and receptors involved in purinergic signaling, we performed qPCR analyses of white adipose tissue (WAT) and BAT isolated from lean and obese mice

  • We detected increased expression of Emr1 in WAT of both dietary and genetic models of obesity (Fig. 1a). This inflammatory response in WAT of these mice was associated with the increased gene expression of the purinergic receptors P2rx4, P2rx5, and P2rx7 as well as marked changes in gene expression levels of nucleotidemetabolizing enzymes CD39 but not Cd38, CD73, and Ucp1 (Fig. 1a)

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Summary

Introduction

Adipose tissue is a complex organ with an important role in endocrine, metabolic, and immune regulatory processes. There are two types of adipose tissues: white adipose tissue (WAT) composed of white adipocytes that stores energy in the form of triglycerides and brown adipose tissue. Adipose tissue mRNA as well as circulating CCL2 and IL6 levels correlate positively with the degree of corpulence and insulin resistance in obese mice and humans [9,10,11,12]

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