Mutation of a Src phosphorylation site in the PDGF beta-receptor leads to increased PDGF-stimulated chemotaxis but decreased mitogenesis.

Klaus Hansen; M Johnell; A Siegbahn; C Rorsman; U Engström; C Wernstedt; C H Heldin; L Rönnstrand

Mutation of a Src phosphorylation site in the PDGF beta-receptor leads to increased PDGF-stimulated chemotaxis but decreased mitogenesis.

Klaus Hansen, M Johnell, A Siegbahn, C Rorsman, U Engström, C Wernstedt, C H Heldin, L Rönnstrand

104 Citationer (Scopus)

Abstract

Udgivelsesdato: 1996-Oct-1

Originalsprog	Engelsk
Tidsskrift	EMBO Journal
Vol/bind	15
Udgave nummer	19
Sider (fra-til)	5299-313
Antal sider	14
ISSN	0261-4189
Status	Udgivet - 1996

Citationsformater

@article{12c8a700532811dd8d9f000ea68e967b,

title = "Mutation of a Src phosphorylation site in the PDGF beta-receptor leads to increased PDGF-stimulated chemotaxis but decreased mitogenesis.",

abstract = "Ligand induced activation of the beta-receptor for platelet-derived growth factor (PDGF) leads to activation of Src family tyrosine kinases. We have explored the possibility that the receptor itself is a substrate for Src. We show that Tyr934 in the kinase domain of the PDGF receptor is phosphorylated by Src. Cell lines expressing a beta-receptor mutant, in which Tyr934 was replaced with a phenyalanine residue, showed reduced mitogenic signaling in response to PDGF-BB. In contrast, the mutant receptor mediated increased signals for chemotaxis and actin reorganization. Whereas the motility responses of cells expressing wild-type beta-receptors were attenuated by inhibition of phosphatidylinositol 3'-kinase, those of cells expressing the mutant receptor were only slightly influenced. In contrast, PDGF-BB-induced chemotaxis of the cells with the mutant receptor was attenuated by inhibition of protein kinase C, whereas the chemotaxis of cells expressing the wild-type beta-receptor was less affected. Moreover, the PDGF-BB-stimulated tyrosine phosphorylation of phospholipase C-gamma was increased in the mutant receptor cells compared with wild-type receptor cells. In conclusion, the characteristics of the Y934F mutant suggest that the phosphorylation of Tyr934 by Src negatively modulates a signal transduction pathway leading to motility responses which involves phospholipase C-gamma, and shifts the response to increased mitogenicity.",

author = "Klaus Hansen and M Johnell and A Siegbahn and C Rorsman and U Engstr{\"o}m and C Wernstedt and Heldin, {C H} and L R{\"o}nnstrand",

note = "Keywords: 1-Phosphatidylinositol 3-Kinase; Actins; Amino Acid Sequence; Cell Division; Cell Line; Chemotaxis; Chromones; Enzyme Inhibitors; Hela Cells; Humans; Isoenzymes; Kinetics; Molecular Sequence Data; Morpholines; Mutation; Peptides; Phospholipase C gamma; Phosphorylation; Phosphotransferases (Alcohol Group Acceptor); Platelet-Derived Growth Factor; Protein Binding; Protein Kinase C; Proto-Oncogene Proteins pp60(c-src); Receptor, Platelet-Derived Growth Factor beta; Receptors, Platelet-Derived Growth Factor; Recombinant Fusion Proteins; Signal Transduction; Type C Phospholipases; Tyrosine; src Homology Domains",

year = "1996",

language = "English",

volume = "15",

pages = "5299--313",

journal = "EMBO Journal",

issn = "0261-4189",

publisher = "Wiley-Blackwell",

number = "19",

}

TY - JOUR

T1 - Mutation of a Src phosphorylation site in the PDGF beta-receptor leads to increased PDGF-stimulated chemotaxis but decreased mitogenesis.

AU - Hansen, Klaus

AU - Johnell, M

AU - Siegbahn, A

AU - Rorsman, C

AU - Engström, U

AU - Wernstedt, C

AU - Heldin, C H

AU - Rönnstrand, L

N1 - Keywords: 1-Phosphatidylinositol 3-Kinase; Actins; Amino Acid Sequence; Cell Division; Cell Line; Chemotaxis; Chromones; Enzyme Inhibitors; Hela Cells; Humans; Isoenzymes; Kinetics; Molecular Sequence Data; Morpholines; Mutation; Peptides; Phospholipase C gamma; Phosphorylation; Phosphotransferases (Alcohol Group Acceptor); Platelet-Derived Growth Factor; Protein Binding; Protein Kinase C; Proto-Oncogene Proteins pp60(c-src); Receptor, Platelet-Derived Growth Factor beta; Receptors, Platelet-Derived Growth Factor; Recombinant Fusion Proteins; Signal Transduction; Type C Phospholipases; Tyrosine; src Homology Domains

PY - 1996

Y1 - 1996

N2 - Ligand induced activation of the beta-receptor for platelet-derived growth factor (PDGF) leads to activation of Src family tyrosine kinases. We have explored the possibility that the receptor itself is a substrate for Src. We show that Tyr934 in the kinase domain of the PDGF receptor is phosphorylated by Src. Cell lines expressing a beta-receptor mutant, in which Tyr934 was replaced with a phenyalanine residue, showed reduced mitogenic signaling in response to PDGF-BB. In contrast, the mutant receptor mediated increased signals for chemotaxis and actin reorganization. Whereas the motility responses of cells expressing wild-type beta-receptors were attenuated by inhibition of phosphatidylinositol 3'-kinase, those of cells expressing the mutant receptor were only slightly influenced. In contrast, PDGF-BB-induced chemotaxis of the cells with the mutant receptor was attenuated by inhibition of protein kinase C, whereas the chemotaxis of cells expressing the wild-type beta-receptor was less affected. Moreover, the PDGF-BB-stimulated tyrosine phosphorylation of phospholipase C-gamma was increased in the mutant receptor cells compared with wild-type receptor cells. In conclusion, the characteristics of the Y934F mutant suggest that the phosphorylation of Tyr934 by Src negatively modulates a signal transduction pathway leading to motility responses which involves phospholipase C-gamma, and shifts the response to increased mitogenicity.

AB - Ligand induced activation of the beta-receptor for platelet-derived growth factor (PDGF) leads to activation of Src family tyrosine kinases. We have explored the possibility that the receptor itself is a substrate for Src. We show that Tyr934 in the kinase domain of the PDGF receptor is phosphorylated by Src. Cell lines expressing a beta-receptor mutant, in which Tyr934 was replaced with a phenyalanine residue, showed reduced mitogenic signaling in response to PDGF-BB. In contrast, the mutant receptor mediated increased signals for chemotaxis and actin reorganization. Whereas the motility responses of cells expressing wild-type beta-receptors were attenuated by inhibition of phosphatidylinositol 3'-kinase, those of cells expressing the mutant receptor were only slightly influenced. In contrast, PDGF-BB-induced chemotaxis of the cells with the mutant receptor was attenuated by inhibition of protein kinase C, whereas the chemotaxis of cells expressing the wild-type beta-receptor was less affected. Moreover, the PDGF-BB-stimulated tyrosine phosphorylation of phospholipase C-gamma was increased in the mutant receptor cells compared with wild-type receptor cells. In conclusion, the characteristics of the Y934F mutant suggest that the phosphorylation of Tyr934 by Src negatively modulates a signal transduction pathway leading to motility responses which involves phospholipase C-gamma, and shifts the response to increased mitogenicity.

M3 - Journal article

C2 - 8895575

SN - 0261-4189

VL - 15

SP - 5299

EP - 5313

JO - EMBO Journal

JF - EMBO Journal

IS - 19

ER -

Mutation of a Src phosphorylation site in the PDGF beta-receptor leads to increased PDGF-stimulated chemotaxis but decreased mitogenesis.

Abstract

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