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J Biol Chem, Vol. 274, Issue 22, 15480-15486, May 28, 1999
1A
Integrins, and Epidermal Growth Factor or Platelet-derived Growth
Factor in Mediation of Cell Migration
§,
, and
From the GD25 cells lacking the
Departments of Medicine and Biomolecular
Chemistry, University of Wisconsin, Madison, Wisconsin 53706 and
§ Department of Experimental Pathology, Lund University, 221 85 Lund, Sweden
1
integrin subunit or expressing
1A with certain
cytoplasmic mutations have poor directed cell migration to
platelet-derived growth factor (PDGF) or epidermal growth factor (EGF),
ligands of receptor tyrosine kinases, or to lysophosphatidic acid
(LPA), a ligand of G-protein-coupled receptors (Sakai, T., Zhang, Q.,
Fässler, R., and Mosher, D. F. (1998) J. Cell
Biol. 141, 527-538 and Sakai, T., Peyruchaud, O., Fässler,
R., and Mosher, D. F. (1998) J. Biol. Chem. 273, 19378-19382). We demonstrate here that LPA synergizes with signals
induced by
1A integrins and ligated EGF or PDGF
receptors to modulate migration. When LPA was mixed with EGF or PDGF,
migration was greater than with EGF or PDGF alone. The enhancement was
greater for
1A-expressing cells than for
1-null cells. Cells expressing
1A with
mutations of prolines or tyrosines in conserved cytoplasmic
NPXY motifs had blunted migratory responses to mixtures of
LPA and EGF or PDGF. The major effects on
1A-expressing
cells of LPA when combined with EGF or PDGF were to sensitize cells so
that maximal responses were obtained with >10-fold lower
concentrations of growth factor and increase the chemokinetic component
of migration. Sensitization by LPA was lost when cells were
preincubated with pertussis toxin or C3 exotransferase. There was no
evidence for transactivation or sensitization of receptors for EGF or
PDGF by LPA. EGF or PDGF and LPA caused activation of mitogen-activated
protein kinase by pertussis toxin-insensitive and -sensitive pathways
respectively, but activation was not additive. These findings indicate
that signaling pathways initiated by the cytoplasmic domains of ligated
1A integrins and tyrosine kinase receptors interact with
signaling pathways initiated by LPA to facilitate directed cell migration.
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