Blockade of vascular smooth muscle cell proliferation and intimal thickening after balloon injury by the sulfated oligosaccharide PI-88

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dc.contributor.authorFrancis, Dougen_AU
dc.contributor.authorMcGarry, Marken_AU
dc.contributor.authorSantiago, Fernandoen_AU
dc.contributor.authorLowe, Harry Cen_AU
dc.contributor.authorBrown, Ken_AU
dc.contributor.authorBingley, Jen_AU
dc.contributor.authorHayward, Ianen_AU
dc.contributor.authorCowden, Williamen_AU
dc.contributor.authorCampbell, Julie Hen_AU
dc.contributor.authorCampbell, Gordon Ren_AU
dc.contributor.authorChesterman, Cen_AU
dc.contributor.authorKhachigian, Levon Men_AU
dc.contributor.authorParish, Christopheren_AU
dc.date.accessioned2015-12-13T23:13:45Z
dc.date.available2015-12-13T23:13:45Z
dc.date.issued2003
dc.date.updated2015-12-12T08:35:33Z
dc.description.abstractPercutaneous transluminal coronary angioplasty is a frequently used interventional technique to reopen arteries that have narrowed because of atherosclerosis. Restenosis, or renarrowing of the artery shortly after angioplasty, is a major limitation to the success of the procedure and is due mainly to smooth muscle cell accumulation in the artery wall at the site of balloon injury. In the present study, we demonstrate that the antiangiogenic sulfated oligosaccharide, PI-88, inhibits primary vascular smooth muscle cell proliferation and reduces intimal thickening 14 days after balloon angioplasty of rat and rabbit arteries. PI-88 reduced heparan sulfate content in the injured artery wall and prevented change in smooth muscle phenotype. However, the mechanism of PI-88 inhibition was not merely confined to the antiheparanase activity of this compound. PI-88 blocked extracellular signal-regulated kinase-1/2 (ERK1/2) activity within minutes of smooth muscle cell injury. It facilitated FGF-2 release from uninjured smooth muscle cells in vitro, and super-released FGF-2 after injury while inhibiting ERK1/2 activation. PI-88 inhibited the decrease in levels of FGF-2 protein in the rat artery wall within 8 minutes of injury. PI-88 also blocked injury-inducible ERK phosphorylation, without altering the clotting time in these animals. Optical biosensor studies revealed that PI-88 potently inhibited (Ki 10.3 nmol/L) the interaction of FGF-2 with heparan sulfate. These findings show for the first time the capacity of this sulfated oligosaccharide to directly bind FGF-2, block cellular signaling and proliferation in vitro, and inhibit injury-induced smooth muscle cell hyperplasia in two animal models. As such, this study demonstrates a new role for PI-88 as an inhibitor of intimal thickening after balloon angioplasty. The full text of this article is available online at http://www.circresaha.org.
dc.identifier.issn0009-7330
dc.identifier.urihttp://hdl.handle.net/1885/88278
dc.publisherLippincott Williams & Wilkins
dc.sourceCirculation Research
dc.subjectKeywords: fibroblast growth factor 2; heparan sulfate; mitogen activated protein kinase; mitogen activated protein kinase 1; mitogen activated protein kinase 3; oligosaccharide; phosphomannopentaose sulfate; animal; article; binding competition; biological model; b
dc.titleBlockade of vascular smooth muscle cell proliferation and intimal thickening after balloon injury by the sulfated oligosaccharide PI-88
dc.typeJournal article
local.bibliographicCitation.issue8
local.bibliographicCitation.lastpagee77
local.bibliographicCitation.startpagee70
local.contributor.affiliationFrancis, Doug, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationParish, Christopher, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationMcGarry, Mark, University of Queensland
local.contributor.affiliationSantiago, Fernando, University of New South Wales
local.contributor.affiliationLowe, Harry C, University of New South Wales
local.contributor.affiliationBrown, K, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationBingley, J, University of Queensland
local.contributor.affiliationHayward, Ian, University of Queensland
local.contributor.affiliationCowden, William, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationCampbell, Julie H, University of Queensland
local.contributor.affiliationCampbell, Gordon R, University of Queensland
local.contributor.affiliationChesterman, C, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationKhachigian, Levon M, University of New South Wales
local.contributor.authoruidFrancis, Doug, a103731
local.contributor.authoruidParish, Christopher, u6900322
local.contributor.authoruidBrown, K, u880147
local.contributor.authoruidCowden, William, u7901248
local.contributor.authoruidChesterman, C, v001725
local.description.notesImported from ARIES
local.description.refereedYes
local.identifier.absfor110704 - Cellular Immunology
local.identifier.ariespublicationMigratedxPub17899
local.identifier.citationvolume92
local.identifier.scopusID2-s2.0-0038284090
local.type.statusPublished Version

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