The adrenergic-induced ERK3 pathway drives lipolysis and suppresses energy dissipation.
Rabih El- MerahbiJonathan Trujillo VieraAngel Loza ValdesKatarzyna KolczynskaSaskia ReuterMona C LöfflerManuela ErkCarsten P AdeTill KarwenAlexander E MayerMartin EilersGrzegorz SumaraPublished in: Genes & development (2020)
Obesity-induced diabetes affects >400 million people worldwide. Uncontrolled lipolysis (free fatty acid release from adipocytes) can contribute to diabetes and obesity. To identify future therapeutic avenues targeting this pathway, we performed a high-throughput screen and identified the extracellular-regulated kinase 3 (ERK3) as a hit. We demonstrated that β-adrenergic stimulation stabilizes ERK3, leading to the formation of a complex with the cofactor MAP kinase-activated protein kinase 5 (MK5), thereby driving lipolysis. Mechanistically, we identified a downstream target of the ERK3/MK5 pathway, the transcription factor FOXO1, which promotes the expression of the major lipolytic enzyme ATGL. Finally, we provide evidence that targeted deletion of ERK3 in mouse adipocytes inhibits lipolysis, but elevates energy dissipation, promoting lean phenotype and ameliorating diabetes. Thus, ERK3/MK5 represents a previously unrecognized signaling axis in adipose tissue and an attractive target for future therapies aiming to combat obesity-induced diabetes.
Keyphrases
- adipose tissue
- signaling pathway
- insulin resistance
- type diabetes
- pi k akt
- cell proliferation
- transcription factor
- glycemic control
- high throughput
- protein kinase
- cardiovascular disease
- high fat diet induced
- metabolic syndrome
- high glucose
- high fat diet
- weight loss
- diabetic rats
- fatty acid
- weight gain
- current status
- oxidative stress
- drug induced
- cancer therapy
- skeletal muscle
- body mass index
- bone mineral density
- body composition
- drug delivery