IP-10 Inhibits Epidermal Growth Factor–induced Motility by Decreasing Epidermal Growth Factor Receptor–mediated Calpain Activity

doi:10.1083/jcb.146.1.243

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J. Cell Biol., Volume 146, Number 1, July 12, 1999 243-254
Copyright © 1999 by The Rockefeller University Press.

IP-10 Inhibits Epidermal Growth Factor–induced Motility by Decreasing Epidermal Growth Factor Receptor–mediated Calpain Activity

Hidenori Shiraha^a, Angela Glading^a, Kiran Gupta^a,b, and Alan Wells^a,b
^a Department of Pathology, University of Alabama at Birmingham, Birmingham, Alabama 35294-0007
^b Birmingham Veterans Affairs Medical Center, Birmingham, Alabama 35233

Correspondence to: Alan Wells, Department of Pathology, Scaife 713, University of Pittsburgh, Pittsburgh, PA 15261., wellsa{at}msx.upmc.edu (E-mail), (412) 648-9550 (phone)

During wound healing, fibroblasts are recruited from the surroundingtissue to accomplish repair. The requisite migration and proliferationof the fibroblasts is promoted by growth factors including thosethat activate the epidermal growth factor receptor (EGFR). Counterstimulatoryfactors in wound fluid are postulated to limit this response;among these factors is the ELR-negative CXC chemokine, interferoninducible protein-10 (IP-10). We report here that IP-10 inhibitedEGF- and heparin-binding EGF-like growth factor–inducedHs68 human dermal fibroblast motility in a dose-dependent manner(to 52% and 44%, respectively, at 50 ng/ml IP-10), whereas IP-10had no effect on either basal or EGFR-mediated mitogenesis (96± 15% at 50 ng/ml). These data demonstrate for the firsttime a counterstimulatory effect of IP-10 on a specific inducedfibroblast response, EGFR-mediated motility.

To define the molecular basis of this negative transmodulationof EGFR signaling, we found that IP-10 did not adversely impactreceptor or immediate postreceptor signaling as determined bytyrosyl phosphorylation of EGFR and two major downstream effectorsphospholipase C- ${gamma}$ and erk mitogen-activated protein kinases.Morphological studies suggested which biophysical steps maybe affected by demonstrating that IP-10 treatment resulted inan elongated cell morphology reminiscent of failure to detachthe uropod; in support of this, IP-10 pretreatment inhibitedEGF-induced cell detachment. These data suggested that calpainactivity may be involved. The cell permeant agent, calpain inhibitorI, limited EGF-induced motility and de-adhesion similarly toIP-10. IP-10 also prevented EGF- induced calpain activation(reduced by 71 ± 7%). That this inhibition of EGF-inducedcalpain activity was secondary to IP-10 initiating a cAMP-proteinkinase A-calpain cascade is supported by the following evidence:(a) the cell permeant analogue 8-(4-chlorophenylthio)-cAMP (CPT-cAMP)prevented EGF-induced calpain activity and motility; (b) otherELR-negative CXC chemokines, monokine induced by IFN- ${gamma}$ and plateletfactor 4 that also generate cAMP, inhibited EGF-induced cellmigration and calpain activation; and (c) the protein kinaseA inhibitor Rp-8-Br-cAMPS abrogated IP-10 inhibition of cellmigration, cell detachment, and calpain activation. Our findingsprovide a model by which IP-10 suppresses EGF-induced cell motilityby inhibiting EGF-induced detachment of the trailing edges ofmotile cells.

Key Words: EGF receptor, cell motility, calpain, chemokine, fibroblasts

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