Evidence from studies in rodents and in isolated adipocytes that agonists of the chemerin receptor CMKLR1 may be beneficial in the treatment of type 2 diabetes

Edward T Wargent; Mohamed S Zaibi; Jacqueline F O'Dowd; Michael A Cawthorne; Steven J Wang; Jonathan R S Arch; Claire J Stocker

doi:10.7717/peerj.753

Evidence from studies in rodents and in isolated adipocytes that agonists of the chemerin receptor CMKLR1 may be beneficial in the treatment of type 2 diabetes

PeerJ. 2015 Feb 5:3:e753. doi: 10.7717/peerj.753. eCollection 2015.

Authors

Edward T Wargent¹, Mohamed S Zaibi¹, Jacqueline F O'Dowd¹, Michael A Cawthorne¹, Steven J Wang², Jonathan R S Arch¹, Claire J Stocker¹

Affiliations

¹ Clore Laboratory, Buckingham Institute for Translational Medicine, University of Buckingham , Buckingham , UK.
² AstraZeneca R & D, Alderley Park , Macclesfield , UK.

Abstract

The literature is unclear on whether the adipokine chemerin has pro- or anti-inflammatory properties or plays any role in the aetiology of type 2 diabetes or obesity. To address these questions, and in particular the potential of agonists or antagonists of the chemerin receptor CMKLR1 in the treatment of type 2 diabetes and obesity, we studied the metabolic phenotypes of both male and female, CMKLR1 knockout and heterozygote mice. We also investigated changes in plasma chemerin levels and chemerin gene mRNA content in adipose tissue in models of obesity and diabetes, and in response to fasting or administration of the insulin sensitizing drug rosiglitazone, which also has anti-inflammatory properties. The effects of murine chemerin and specific C-terminal peptides on glucose uptake in wild-type and CMKLR1 knockout adipocytes were investigated as a possible mechanism by which chemerin affects the blood glucose concentration. Both male and female CMKLR1 knockout and heterozygote mice displayed a mild tendency to obesity and impaired glucose homeostasis, but only when they were fed on a high-fat died, rather than a standard low-fat diet. Obesity and impaired glucose homeostasis did not occur concurrently, suggesting that obesity was not the sole cause of impaired glucose homeostasis. Picomolar concentrations of chemerin and its C15- and C19-terminal peptides stimulated glucose uptake in the presence of insulin by rat and mouse wild-type epididymal adipocytes, but not by murine CMKLR1 knockout adipocytes. The insulin concentration-response curve was shifted to the left in the presence of 40 pM chemerin or its C-15 terminal peptide. The plasma chemerin level was raised in diet-induced obesity and ob/ob but not db/db mice, and was reduced by fasting and, in ob/ob mice, by treatment with rosiglitazone. These findings suggest that an agonist of CMKLR1 is more likely than an antagonist to be of value in the treatment of type 2 diabetes and to have associated anti-obesity and anti-inflammatory activities. One mechanism by which an agonist of CMKLR1 might improve glucose homeostasis is by increasing insulin-stimulated glucose uptake by adipocytes.

Keywords: Adipocyte; Chemerin; Chemerin receptor; Glucose uptake; Obesity; Rosiglitazone; Type 2 diabetes.

Grants and funding

AstraZeneca funded most of the work described in this manuscript (grant 20080509LL/SEML-7DSHX3). Some of the glucose uptake work was funded from the resources of the Clore Laboratory after the formal collaboration with AstraZeneca ended. The original idea to work in this area was Steven Wang’s. He had moved from the Clore Laboratory to work for AstraZeneca, who had chemerin receptor knockout mice available to them. The details of the experiments were designed by University of Buckingham authors but discussed with Steven Wang to solicit his input. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.