Modulation of Glutamine Metabolism by the PI(3)K-PKB-FOXO Network Regulates Autophagy

Overview

Journal Nat Cell Biol

Specialty Cell Biology

Date 2012 Jul 24

PMID 22820375

Citations 130

Authors

Kristan E van der Vos

Pernilla Eliasson

Tassula Proikas-Cezanne

Stephin J Vervoort

Ruben van Boxtel

Marrit Putker

Iris J van Zutphen

Mario Mauthe

Sebastian Zellmer

Cornelieke Pals

Liesbeth P Verhagen

Marian J A Groot Koerkamp

A Koen Braat

Tobias B Dansen

Frank C Holstege

Rolf Gebhardt

Boudewijn M Burgering

Paul J Coffer

Affiliations

Soon will be listed here.

Abstract

The PI(3)K-PKB-FOXO signalling network provides a major intracellular hub for the regulation of cell proliferation, survival and stress resistance. Here we report an unexpected role for FOXO transcription factors in regulating autophagy by modulating intracellular glutamine levels. To identify transcriptional targets of this network, we performed global transcriptional analyses after conditional activation of the key components PI(3)K, PKB/Akt, FOXO3 and FOXO4. Using this pathway approach, we identified glutamine synthetase as being transcriptionally regulated by PI(3)K-PKB-FOXO signalling. Conditional activation of FOXO also led to an increased level of glutamine production. FOXO activation resulted in mTOR inhibition by preventing the translocation of mTOR to lysosomal membranes in a glutamine-synthetase-dependent manner. This resulted in an increased level of autophagy as measured by LC3 lipidation, p62 degradation and fluorescent imaging of multiple autophagosomal markers. Inhibition of FOXO3-mediated autophagy increased the level of apoptosis, suggesting that the induction of autophagy by FOXO3-mediated glutamine synthetase expression is important for cellular survival. These findings reveal a growth-factor-responsive network that can directly modulate autophagy through the regulation of glutamine metabolism.

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