The anorexic effect of Ex4/Fc through GLP-1 receptor activation in high-fat diet fed mice

Exendin-4 （Ex4）, a peptide initially found in the saliva of the Gila monster, can activate the signaling pathway of the incre- tin hormone glucagon-like peptide-1 （GLP-1） through the GLP-1 receptor （GLP-1R）. We previously reported that a chimera protein consisting of Ex4 and mouse IgG heavy chain constant regions （Ex4/Fc） can exert biological effects of GLP-1, such as improving glycemic control and ameliorating manifestations in diabetic mice. The aim of this study was to determine whether Ex4/Fc is effective in modulating energy homeostasis in mice. Our results showed that in vivo expres- sion of Ex4/Fc by intramuscular injection of the plasmid en- coding Ex4/Fc followed by local electroporation effectively decreased food intake in the mice on high-fat diet （HFD） feeding. In addition, the reduced energy intake was associated with the decreased excrements from the Ex4/Fc-treated HFD mice but not the Fc control mice. Remarkably, the Ex4/Fc- treated HFD mice displayed significantly lower triglyceride （TG） levels when compared with the control mice. Interest- ingly, while the leptin levels were not changed, the circulating ghrelin levels were higher in Ex4/Fc mice than those in the Fc control mice. These results suggested that Ex4/Fc can improve energy metabolism and lipid metabolism through GLP-1R in mice under excessive nutrition conditions.