RT Journal Article SR Electronic T1 Egr1 deficiency induces browning of inguinal subcutaneous white adipose tissue in mice JF bioRxiv FD Cold Spring Harbor Laboratory SP 150003 DO 10.1101/150003 A1 Cécile Milet A1 Marianne Bléher A1 Kassandra Allbright A1 Mickael Orgeur A1 Fanny Coulpier A1 Delphine Duprez A1 Emmanuelle Havis YR 2017 UL http://biorxiv.org/content/early/2017/07/01/150003.abstract AB Beige adipocyte differentiation within white adipose tissue, referred to as browning, is seen as a possible mechanism for increasing energy expenditure. The molecular regulation underlying the thermogenic browning process has not been entirely elucidated. Here, we identify the zinc finger transcription factor EGR1 as a negative regulator of the beige fat program. Loss of Egr1 in mice promotes browning in the absence of external stimulation and activates Ucp1 that encodes the key thermogenic mitochondrial uncoupling protein-1. Moreover, EGR1 is recruited to the proximal region of the Ucp1 promoter in subcutaneous inguinal white adipose tissue. Transcriptomic analysis of subcutaneous inguinal white adipose tissue in the absence of Egr1 identifies the molecular signature of white adipocyte browning downstream of Egr1 deletion and highlights a concomitant increase of beige differentiation marker and decrease in extracellular matrix gene expression. Conversely, Egr1 overexpression in mesenchymal stem cells decreases beige adipocyte differentiation, while increasing extracellular matrix production. These results uncover the role of Egr1 in blocking energy expenditure via direct Ucp1 transcription regulation and highlight Egr1 as a therapeutic target for counteracting obesity.