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Macrophage-derived human resistin exacerbates adipose tissue inflammation and insulin resistance in mice
Mohammed Qatanani, … , Rexford S. Ahima, Mitchell A. Lazar
Mohammed Qatanani, … , Rexford S. Ahima, Mitchell A. Lazar
Published February 2, 2009
Citation Information: J Clin Invest. 2009;119(3):531-539. https://doi.org/10.1172/JCI37273.
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Research Article Metabolism

Macrophage-derived human resistin exacerbates adipose tissue inflammation and insulin resistance in mice

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Abstract

Resistin is an adipokine that contributes to insulin resistance in mice. In humans, however, studies investigating the link between resistin and metabolic disease are conflicting. Further complicating the matter, human resistin is produced mainly by macrophages rather than adipocytes. To address this important issue, we generated mice that lack adipocyte-derived mouse resistin but produce human resistin in a pattern similar to that found in humans, i.e., in macrophages (humanized resistin mice). When placed on a high-fat diet, the humanized resistin mice rapidly developed accelerated white adipose tissue (WAT) inflammation, leading to increased lipolysis and increased serum free fatty acids. Over time, these mice accumulated lipids, including diacylglycerols, in muscle. We found that this resulted in increased Pkcq pathway activity, leading to increased serine phosphorylation of Irs-1 and insulin resistance. Thus, although the site of resistin production differs between species, human resistin exacerbates WAT inflammation and contributes to insulin resistance.

Authors

Mohammed Qatanani, Nava R. Szwergold, David R. Greaves, Rexford S. Ahima, Mitchell A. Lazar

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Plasma metabolic profile of humanized resistin mice on high-fat diet for...

Plasma metabolic profile of humanized resistin mice on high-fat diet for 4 days


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