Regulation of EphA 4 Kinase Activity is Required for a Subset of Axon Guidance Decisions Suggesting a Key Role for Receptor Clustering in Eph Function

Overview

Journal Neuron

Publisher Cell Press

Specialty Neurology

Date 2005 Aug 17

PMID 16102535

Citations 60

Authors

Joaquim Egea

Ulla Vig Nissen

Audrey Dufour

Mustafa Sahin

Paul Greer

Klas Kullander

Thomas D Mrsic-Flogel

Michael E Greenberg

Ole Kiehn

Pierre Vanderhaeghen

Rudiger Klein

Affiliations

Soon will be listed here.

Abstract

Signaling by receptor tyrosine kinases (RTKs) is mediated by their intrinsic kinase activity. Typically, kinase-activating mutations result in ligand-independent signaling and gain-of-function phenotypes. Like other RTKs, Ephs require kinase activity to signal, but signaling by Ephs in vitro also requires clustering by their membrane bound ephrin ligands. The relative importance of Eph kinase activity and clustering for in vivo functions is unknown. We find that knockin mice expressing a mutant form of EphA4 (EphA4(EE)), whose kinase is constitutively activated in the absence of ephrinB ligands, are deficient in the development of thalamocortical projections and some aspects of central pattern generator rhythmicity. Surprisingly, other functions of EphA4 were regulated normally by EphA4(EE), including midline axon guidance, hindlimb locomotion, in vitro growth cone collapse, and phosphorylation of ephexin1. These results suggest that signaling of Eph RTKs follows a multistep process of induced kinase activity and higher-order clustering different from RTKs responding to soluble ligands.

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