Litcius/Paper detail

Akt phosphorylates insulin receptor substrate to limit PI3K-mediated PIP3 synthesis

Alison L. Kearney, Dougall M. Norris, Milad Ghomlaghi, Martin Kin Lok Wong, Sean J. Humphrey, Luke Carroll, Guang Yang, Kristen C. Cooke, Pengyi Yang, Thomas A. Geddes, Sung‐Young Shin, Daniel J. Fazakerley, Lan K. Nguyen, David E. James, James G. Burchfield

2021eLife85 citationsDOIOpen Access PDF

Abstract

The phosphoinositide 3-kinase (PI3K)-Akt network is tightly controlled by feedback mechanisms that regulate signal flow and ensure signal fidelity. A rapid overshoot in insulin-stimulated recruitment of Akt to the plasma membrane has previously been reported, which is indicative of negative feedback operating on acute timescales. Here, we show that Akt itself engages this negative feedback by phosphorylating insulin receptor substrate (IRS) 1 and 2 on a number of residues. Phosphorylation results in the depletion of plasma membrane-localised IRS1/2, reducing the pool available for interaction with the insulin receptor. Together these events limit plasma membrane-associated PI3K and phosphatidylinositol (3,4,5)-trisphosphate (PIP3) synthesis. We identified two Akt-dependent phosphorylation sites in IRS2 at S306 (S303 in mouse) and S577 (S573 in mouse) that are key drivers of this negative feedback. These findings establish a novel mechanism by which the kinase Akt acutely controls PIP3 abundance, through post-translational modification of the IRS scaffold.

Topics & Concepts

Protein kinase BPI3K/AKT/mTOR pathwayPhosphorylationProto-Oncogene Proteins c-aktCell biologyIRS1Insulin receptorIRS2PhosphatidylinositolSignal transductionBiologyInsulinChemistryEndocrinologyInsulin resistancePancreatic function and diabetesPI3K/AKT/mTOR signaling in cancerMetabolism, Diabetes, and Cancer