%0 Journal Article %A Eric S. Muise %A Barbara Azzolina %A David W. Kuo %A Mohamed El-Sherbeini %A Yejun Tan %A Xiling Yuan %A James Mu %A John R. Thompson %A Joel P. Berger %A Kenny K. Wong %T Adipose Fibroblast Growth Factor 21 Is Up-Regulated by Peroxisome Proliferator-Activated Receptor γ and Altered Metabolic States %D 2008 %R 10.1124/mol.108.044826 %J Molecular Pharmacology %P 403-412 %V 74 %N 2 %X Adipose tissue is a metabolically responsive endocrine organ that secretes a myriad of adipokines. Antidiabetic drugs such as peroxisome proliferator-activated receptor (PPAR) γ agonists target adipose tissue gene expression and correct hyperglycemia via whole-body insulin sensitization. The mechanism by which altered gene expression in adipose tissue affects liver and muscle insulin sensitivity (and thus glucose homeostasis) is not fully understood. One possible mechanism involves the alteration in adipokine secretion, in particular the up-regulation of secreted factors that increase whole-body insulin sensitivity. Here, we report the use of transcriptional profiling to identify genes encoding for secreted proteins the expression of which is regulated by PPARγ agonists. Of the 379 genes robustly regulated by two structurally distinct PPARγ agonists in the epididymal white adipose tissue (EWAT) of db/db mice, 33 encoded for known secreted proteins, one of which was FGF21. Although FGF21 was recently reported to be up-regulated in cultured adipocytes by PPARγ agonists and in liver by PPARα agonists and induction of ketotic states, we demonstrate that the protein is transcriptionally up-regulated in adipose tissue in vivo by PPARγ agonist treatment and under a variety of physiological conditions, including fasting and high fat diet feeding. In addition, we found that circulating levels of FGF21 protein were increased upon treatment with PPARγ agonists and under ketogenic states. These results suggest a role for FGF21 in mediating the antidiabetic activities of PPARγ agonists. The American Society for Pharmacology and Experimental Therapeutics %U https://molpharm.aspetjournals.org/content/molpharm/74/2/403.full.pdf