Fibroblast growth factor 21 is not required for the antidiabetic actions of the thiazoladinediones

Fibroblast growth factor 21 is an emerging metabolic regulator that was recently proposed to be a fed-state inducible factor in adipose tissue. As mice lacking FGF21 were refractory to treatment with rosiglitazone, FGF21 was suggested to underlie PPAR gamma-driven pharmacology and side effect profile (Dutchak et al., 2012 [12]). To evaluate FGF21/PPAR gamma cross-talk we conducted experiments in control and FGF21 null animals and found that rosiglitazone was equally efficacious in both strains. Specifically, diverse endpoints ranging from enhanced glycemic control, improved lipid homeostasis and side effects such as adipose accumulation were evident in both genotypes. Furthermore, the transcriptional signature and cytokine secretion profile of rosiglitazone action were maintained in our FGF21K0 animals. Finally, we found that FGF21 in adipose was expressed at comparable levels in fasted and fed states. Thus, our data present a new viewpoint on the FGF21/PPAR gamma interplay whereby FGF21 is not necessary for the metabolic events downstream of PPAR gamma. (C) 2013 Elsevier GmbH. Open access under CC BY-NC ND license