PAK4 Phosphorylates and Inhibits AMPKα to Control Glucose Uptake

Overview

Journal Nat Commun

Specialty Biology

Date 2024 Aug 10

PMID 39127697

Authors

Dandan Wu

Hwang Chan Yu

Hye-Na Cha

Soyoung Park

Yoonji Lee

Sun-Jung Yoon

So-Young Park

Byung-Hyun Park

Eun Ju Bae

Affiliations

Soon will be listed here.

Abstract

Our recent studies have identified p21-activated kinase 4 (PAK4) as a key regulator of lipid catabolism in the liver and adipose tissue, but its role in glucose homeostasis in skeletal muscle remains to be explored. In this study, we find that PAK4 levels are highly upregulated in the skeletal muscles of diabetic humans and mice. Skeletal muscle-specific Pak4 ablation or administering the PAK4 inhibitor in diet-induced obese mice retains insulin sensitivity, accompanied by AMPK activation and GLUT4 upregulation. We demonstrate that PAK4 promotes insulin resistance by phosphorylating AMPKα2 at Ser491, thereby inhibiting AMPK activity. We additionally show that skeletal muscle-specific expression of a phospho-mimetic mutant AMPKα2 impairs glucose tolerance, while the phospho-inactive mutant AMPKα2 improves it. In summary, our findings suggest that targeting skeletal muscle PAK4 may offer a therapeutic avenue for type 2 diabetes.

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