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Horm Metab Res 2007; 39(4): 244-249
DOI: 10.1055/s-2007-972577
Original Basic

© Georg Thieme Verlag KG Stuttgart · New York

Expression of Chemokine Receptors in Insulin-resistant Human Skeletal Muscle Cells

H. Sell 1 [*] , U. Kaiser 1 [*] , J. Eckel 1
  • 1Institute of Clinical Biochemistry and Pathobiochemistry, German Diabetes Center, Düsseldorf, Germany
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Publikationsverlauf

received 2. 10. 2006

accepted 11. 1. 2007

Publikationsdatum:
19. April 2007 (online)

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Abstract

Adipokines including chemokines are able to induce insulin resistance in human skeletal muscle cells, which may also be relevant for the observed link between obesity and diabetes. This study is aimed to analyze the expression of chemokine CC motif receptors (CCRs) in the insulin-resistant state in human skeletal muscle cells. Differentiated skeletal muscle cells were incubated for 24-72 hours with high concentrations of glucose and insulin (GI) or TNFα. In addition, myocytes were co-stimulated with monocyte chemotactic protein (MCP)-1 or adipocyte-conditioned medium (CM) and TNFα for 24 and 48 hours. Treatment with GI rapidly induced insulin resistance whereas TNFα impaired insulin signaling in a more chronic fashion (48-72 h). CM and MCP-1 also induced insulin resistance that was, however, not increased by co-stimulation with TNFα. Expression of CCR2 was decreased during differentiation but up-regulated in insulin-resistant myocytes after treatment with GI (24-72 h) and TNFα (72 h). Expression of CCR4 and CCR10 was down-regulated after treatment with TNFα, MCP-1, and CM. Our data show that the expression of CCR2, CCR4, and CCR10 is differentially regulated by different insulin resistance-inducing treatments in myotubes. However, we could not find a clear correlation between the level of insulin resistance and CCR expression in myotubes. In conclusion, we propose that upregulation of CCR2 in skeletal muscle does not represent a major step leading to muscle insulin resistance.

Key words

insulin resistance - skeletal muscle - chemokine receptor

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1 These authors contributed equally to this work.

Correspondence

Prof. Dr. J. Eckel

German Diabetes Center

Auf'm Hennekamp 65

40225 Düsseldorf

Germany

Telefon: +49/211/338 22 40

Fax: +49/211/338 26 97

eMail: eckel@uni-duesseldorf.de

URL: http://www.ddz.uni-duesseldorf.de

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