Feedback in the β-catenin Destruction Complex Imparts Bistability and Cellular Memory

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2023 Jan 4

PMID 36598937

Authors

Mary Jo Cantoria

Elaheh Alizadeh

Janani Ravi

Reeba P Varghese

Nawat Bunnag

Kelvin W Pond

Arminja N Kettenbach

Yashi Ahmed

Andrew L Paek

John J Tyson

Konstantin Doubrovinski

Ethan Lee

Curtis A Thorne

Affiliations

Soon will be listed here.

Abstract

Wnt ligands are considered classical morphogens, for which the strength of the cellular response is proportional to the concentration of the ligand. Herein, we show an emergent property of bistability arising from feedback among the Wnt destruction complex proteins that target the key transcriptional co-activator β-catenin for degradation. Using biochemical reconstitution, we identified positive feedback between the scaffold protein Axin and the kinase glycogen synthase kinase 3 (GSK3). Theoretical modeling of this feedback between Axin and GSK3 suggested that the activity of the destruction complex exhibits bistable behavior. We experimentally confirmed these predictions by demonstrating that cellular cytoplasmic β-catenin concentrations exhibit an "all-or-none" response with sustained memory (hysteresis) of the signaling input. This bistable behavior was transformed into a graded response and memory was lost through inhibition of GSK3. These findings provide a mechanism for establishing decisive, switch-like cellular response and memory upon Wnt pathway stimulation.

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