Literature DB >> 17574222

Autocrine expression of osteopontin contributes to PDGF-mediated arterial smooth muscle cell migration.

Sandra Jalvy1, Marie-Ange Renault, Laetitia Lam Shang Leen, Isabelle Belloc, Jacques Bonnet, Alain-Pierre Gadeau, Claude Desgranges.   

Abstract

OBJECTIVE: Migration of smooth muscle cells (SMCs) from the media to the intima of arteries is involved in intimal thickening. The platelet-derived growth factor (PDGF) BB is recognized as a major migratory factor for arterial SMCs both in vitro and during neointima formation. Since PDGF acts in synergy with the matrix protein osteopontin (OPN) and also induces its expression, the present study was conceived to explore the role of the OPN produced in an autocrine fashion by PDGF-stimulated SMCs in the migration process and to define regulatory mechanisms of OPN expression. METHODS AND
RESULTS: PDGF stimulation of quiescent rat aortic SMCs induced their migration (transfilter assays) and the increase of OPN expression (mRNA and protein assays). Blockade of either OPN expression by a specific short interference RNA (siRNA) or of its function by a blocking antibody decreased the PDGF-stimulated migration by about 70%, demonstrating that autocrine production and excretion of OPN are integral to the PDGF-induced SMC migration. In parallel, SMC stimulation by PDGF also activated the transcription factor CREB essentially through mitogen-activated protein kinase (MAPK) 1/2 and protein kinase A (PKA) pathways. Inhibition of either CREB expression (via siRNA) or function (via dominant-negative CREB) decreased both PDGF-induced SMC migration and OPN expression. SMC transfection with OPN promoter reporter constructs demonstrated that PDGF-induced OPN transcription is mediated by CREB binding to two functional sites of the OPN promoter: a CRE site located at -1403 and an AP-1 site located at -76.
CONCLUSION: The present study demonstrates that the autocrine expression of OPN plays a major role in PDGF-induced SMC migration. It further shows that the transcription factor CREB, activated in PDGF-stimulated SMCs, plays a key role in PDGF-induced SMC migration, probably by regulating OPN expression.

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Year:  2007        PMID: 17574222     DOI: 10.1016/j.cardiores.2007.05.019

Source DB:  PubMed          Journal:  Cardiovasc Res        ISSN: 0008-6363            Impact factor:   10.787


  18 in total

1.  Osteopontin, a missing link in PDGF-induced smooth muscle cell migration.

Authors:  Kristina Boström
Journal:  Cardiovasc Res       Date:  2007-07-04       Impact factor: 10.787

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4.  Direct modulation of the protein kinase A catalytic subunit α by growth factor receptor tyrosine kinases.

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6.  Inflammation and vascular smooth muscle cell dedifferentiation following carotid artery ligation.

Authors:  B Paul Herring; April M Hoggatt; Sarah L Griffith; Jeanette N McClintick; Patricia J Gallagher
Journal:  Physiol Genomics       Date:  2016-12-30       Impact factor: 3.107

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Authors:  Guohong Li; Rong Jin; Russell A Norris; Lin Zhang; Shiyong Yu; Fusheng Wu; Roger R Markwald; Anil Nanda; Simon J Conway; Susan S Smyth; D Neil Granger
Journal:  Atherosclerosis       Date:  2009-07-30       Impact factor: 5.162

Review 8.  The bladder extracellular matrix. Part I: architecture, development and disease.

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Journal:  Nat Rev Urol       Date:  2009-11       Impact factor: 14.432

9.  Wnt-5a-induced phosphorylation of DARPP-32 inhibits breast cancer cell migration in a CREB-dependent manner.

Authors:  Christian Hansen; Jillian Howlin; Anders Tengholm; Oleg Dyachok; Wolfgang F Vogel; Angus C Nairn; Paul Greengard; Tommy Andersson
Journal:  J Biol Chem       Date:  2009-08-03       Impact factor: 5.157

Review 10.  Osteopontin: a multifunctional protein at the crossroads of inflammation, atherosclerosis, and vascular calcification.

Authors:  Hyun-Ju Cho; Hyun-Jai Cho; Hyo-Soo Kim
Journal:  Curr Atheroscler Rep       Date:  2009-05       Impact factor: 5.113

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