| dc.contributor.author | Nalbone, G | fr_FR |
| dc.contributor.author | Alessi, MC | fr_FR |
| dc.contributor.author | Juhan-Vague, I | fr_FR |
| dc.date.accessioned | 2012-08-30T12:34:22Z | |
| dc.date.available | 2012-08-30T12:34:22Z | |
| dc.date.issued | 2001 | fr_FR |
| dc.identifier.citation | Nalbone, G ; Alessi, MC ; Juhan-Vague, I, Système fibrinolytique, métalloproteases et pathologie vasculaire., Med Sci (Paris), 2001, Vol. 17, N° 2; p.170-6 | fr_FR |
| dc.identifier.issn | 1958-5381 | fr_FR |
| dc.identifier.uri | http://hdl.handle.net/10608/1889 | |
| dc.description.abstract | La progression de la plaque d’athérome est un processus
lent et le vaisseau s’adapte à cette modification pour préserver
le plus longtemps possible ses fonctions essentielles
comme une perméabilité sélective, la vasodilatation, la
thromborésistance, tout en isolant de la circulation sanguine
les composants extracellulaires thrombogènes de la
paroi. Lorsque le vaisseau ne parvient plus à s’adapter, les
signes cliniques de la maladie athéromateuse apparaissent
et témoignent d’une perte des propriétés vasorelaxantes et
anti-thrombogènes de la paroi, d’un rétrécissement de la
lumière, conduisant à une fissuration de la plaque avec
risque de thrombose occlusive. Deux systèmes protéolytiques
majeurs travaillent en étroite coopération dans la
paroi vasculaire pour maintenir la structure et les fonctions
normales du vaisseau : le système fibrinolytique ou système
plasminogène/plasmine et le système des métalloprotéases.
L’intervention de ces deux systèmes et leur interaction
contribuent à l’établissement des lésions pariétales responsables
des accidents cardio-vasculaires. | fr |
| dc.description.abstract | Several experimental data obtained from gene invalidation in mice submitted to various vascular injury models (electrical arterial lesion, graft, genetic-induced atherosclerosis) suggest that the interaction between the fibrinolytic and metalloproteinase systems is critical in the development of vascular diseases. Besides its fundamental function to regulate intravascular thrombolysis, the fibrinolytic system is also intimately involved in the regulation of the matrix turnover in the vessel wall and controls in this way important cellular events, such as adhesion, migration and proliferation. This is achieved either directly through the action of plasmin on some matrix proteins such as laminin or fibronectin, or indirectly through the activation of the majority of pro-MMP into active MMP that degrade matrix proteins (laminin, collagene, elastin, gelatin...). PAI-1, independently of its antifibrinolytic property, also directly regulates adhesion and migration processes. These processes are involved in (re)stenosis and in plaque rupture, by acting more specifically on leukocyte infiltration, smooth muscle cell migration, degradation of internal elastic lamina and angiogenesis. Promising therapeutical approaches designed to limit pericellular proteolysis in arterial wall, involve gene transfer therapy and also the class of HMG-CoA reductase inhibitors (statins) that directly regulate the expression of some genes involved in this process. [References: 26] | en |
| dc.language.iso | fr | fr_FR |
| dc.publisher | Masson, Paris | fr_FR |
| dc.rights | Article en libre accès | fr |
| dc.rights | Médecine/Sciences - Inserm - SRMS | fr |
| dc.source | M/S. Médecine sciences [revue papier, ISSN : 0767-0974], 2001, Vol. 17, N° 2; p.170-6 | fr_FR |
| dc.title | Système fibrinolytique, métalloproteases et pathologie vasculaire. | fr |
| dc.title.alternative | Fibrinolytic system, metalloproteinases and vascular diseases. | fr_FR |
| dc.type | Article | fr_FR |
| dc.contributor.affiliation | INSERM EPI 99-36 Faculté de Médecine Timone 27, boulevard Jean Moulin 13385 MARSEILLE CEDEX 05 | - |
| dc.identifier.doi | 10.4267/10608/1889 | |
