Phosphorylation of E3 Ligase Smurf1 Switches Its Substrate Preference in Support of Axon Development

Overview

Journal Neuron

Publisher Cell Press

Specialty Neurology

Date 2011 Jan 26

PMID 21262463

Citations 89

Authors

Pei-Lin Cheng

Hui Lu

Maya Shelly

Hongfeng Gao

Mu-Ming Poo

Affiliations

Soon will be listed here.

Abstract

Ubiquitin E3 ligases serve for ubiquitination of specific substrates, and its ligase efficacy is regulated by interacting proteins or substrate modifications. Whether and how the ligases themselves are modified by cellular signaling is unclear. Here we report that protein kinase A (PKA)-dependent phosphorylation of Smad Ubiquitin Regulatory Factor 1 (Smurf1) can switch its substrate preference between two proteins of opposing actions on axon development. Extracellular factors that promote axon formation elevated Smurf1 phosphorylation at a PKA site Thr³⁰⁶, and preventing this phosphorylation reduced axon formation in cultured hippocampal neurons and impaired polarization of cortical neurons in vivo. Thr³⁰⁶-phosphorylation changed the relative affinities of Smurf1 for its substrates, leading to reduced degradation of polarity protein Par6 and increased degradation of growth-inhibiting RhoA. Thus, PKA-dependent phosphorylation of the E3 ligase could switch its substrate preference, contributing to selective protein degradation required for localized cellular function.

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