Dataset: PPARg agonists induce a white-to-brown fat conversion through stabilization of PRDM16 protein
Brown adipose tissue dissipates energy through heat and functions as a defense against cold and obesity. PPARγ ligands have been shown to...
Brown adipose tissue dissipates energy through heat and functions as a defense against cold and obesity. PPARγ ligands have been shown to induce the browning of white adipocytes; however, the underlying mechanisms remain unclear. Here we show that PPARγ ligands require full agonism to induce a brown fat gene program preferentially in subcutaneous white adipose. These effects require expression of PRDM16, a factor that controls the development of classical brown fat. Depletion of PRDM16 blunts the effects of the PPARγ agonist rosiglitazone on the induced brown fat gene program. Conversely, PRDM16 and rosiglitazone synergistically activate the brown fat gene program in vivo. This synergy is tightly associated with an increased accumulation of PRDM16 protein, due in large measure to an increase in the half-life of the protein in agonist treated cells. Identifying compounds that stabilize PRDM16 protein may represent a novel therapeutic pathway for the treatment of obesity and diabetes. Microarray analysis of the differentiated inguinal adipocytes expressing sh-scr or sh-PRDM16 in the presence or absence of rosiglitazone (1uM). These samples were profiled using Affymetrix mouse 430A_2 arrays, representing 2 biological replicates for each samples (8 samples in total).
- Species:
- mouse
- Samples:
- 8
- Source:
- E-GEOD-35011
- Updated:
- Dec.12, 2014
- Registered:
- Nov.24, 2014
Sample | EXPRESSION | COMPOUND |
---|---|---|
GSM860620 | sh-scr | none |
GSM860620 | sh-scr | none |
GSM860622 | sh-scr | rosiglitazone at 1uM |
GSM860622 | sh-scr | rosiglitazone at 1uM |
GSM860624 | sh-PRDM16 | none |
GSM860624 | sh-PRDM16 | none |
GSM860626 | sh-PRDM16 | rosiglitazone at 1uM |
GSM860626 | sh-PRDM16 | rosiglitazone at 1uM |