Prohibitin/annexin 2 Interaction Regulates Fatty Acid Transport in Adipose Tissue

Overview

Journal JCI Insight

Specialties Biomedical Engineering
General Medicine

Date 2016 Jul 29

PMID 27468426

Citations 43

Authors

Ahmad Salameh

Alexes C Daquinag

Daniela I Staquicini

Zhiqiang An

Katherine A Hajjar

Renata Pasqualini

Wadih Arap

Mikhail G Kolonin

Affiliations

Soon will be listed here.

Abstract

We have previously identified prohibitin (PHB) and annexin A2 (ANX2) as proteins interacting on the surface of vascular endothelial cells in white adipose tissue (WAT) of humans and mice. Here, we demonstrate that ANX2 and PHB also interact in adipocytes. Mice lacking ANX2 have normal WAT vascularization, adipogenesis, and glucose metabolism but display WAT hypotrophy due to reduced fatty acid uptake by WAT endothelium and adipocytes. By using cell culture systems in which ANX2/PHB binding is disrupted either genetically or through treatment with a blocking peptide, we show that fatty acid transport efficiency relies on this protein complex. We also provide evidence that the interaction between ANX2 and PHB mediates fatty acid transport from the endothelium into adipocytes. Moreover, we demonstrate that ANX2 and PHB form a complex with the fatty acid transporter CD36. Finally, we show that the colocalization of PHB and CD36 on adipocyte surface is induced by extracellular fatty acids. Together, our results suggest that an unrecognized biochemical interaction between ANX2 and PHB regulates CD36-mediated fatty acid transport in WAT, thus revealing a new potential pathway for intervention in metabolic diseases.

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