BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. SIRT1, G-protein-coupled receptor binding, HIV infection, Breast, Nosology, Bleomycin)
Bookmark Forward

Prostanoid and TP-receptors in atherothrombosis: is there a role for their antagonism?

Chiara Giannarelli, M Urooj Zafar, Juan J Badimon

AtheroThrombosis Research Unit, Cardiovascular Institute, Mount Sinai School of Medicine, New York, New York 10029, USA.

Thrombosis and haemostasis 2010 Nov


filter terms:
  • adhesion molecules cell (1)
  • animals (1)
  • aspirin (1)
  • attention (1)
  • cardiovascular agents (2)
  • causes of mortality (1)
  • cells (1)
  • contraction (1)
  • endothelial cells (1)
  • endothelin 1 (1)
  • endothelium (1)
  • f2 isoprostanes (1)
  • humans (1)
  • inhibition (3)
  • inhibitors prostaglandin (2)
  • initiation (1)
  • macrophages (2)
  • morbidity (1)
  • muscle smooth (1)
  • muscle smooth, vascular (1)
  • myocardial infarction (1)
  • pgg2 (2)
  • pgh2 (4)
  • platelet (2)
  • platelet activation (2)
  • platelet aggregation (1)
  • platelet aggregation inhibitors (2)
  • platelet function (1)
  • prostanoid receptors (1)
  • prostanoids (5)
  • receptors prostaglandin (2)
  • receptors thromboxane a2 (2)
  • signal transduction (1)
  • smooth muscle cell (2)
  • stroke (1)
  • thrombosis (1)
  • thromboxane a2 (7)
  • tp receptors (7)
  • vasoconstriction (1)
    • Sizes of these terms reflect their relevance to your search.

    Atherosclerosis and its clinical manifestations (i.e. myocardial infarction, stroke) are major causes of mortality and morbidity in Western countries. Endothelial dysfunction is considered the first step in the cascade leading up to coronary events. Increasing evidence suggests that direct inhibition of thromboxane A2/prostaglandin (TP)-receptors may not only have anti-platelet effects but also impact endothelial dysfunction as well as inflammatory component of atherosclerosis. While TP-receptor involvement in platelet function has received the greatest attention, more recent findings support the critical role of TP-receptor in other pathophysiological aspects of atherothrombosis. Prostanoids (i.e. TxA2, F2-isoprostanes, prostaglandins endoperoxides PGG2/PGH2) are known to promote the initiation and progression of atherosclerosis, not only via platelet activation, but through leukocyte-endothelial interactions and vasoconstriction. Dysfunctional endothelium, characterised by increased COX-activity, releases prostanoids that promote endothelial exposure to adhesion molecules and induce smooth muscle cell contraction. Plaque macrophages synthesise PGH2/PGG2 via COX-2; these potent prostanoids can trigger platelet activation and aggregation despite COX-1 inhibition by aspirin. TP-receptor inhibition has been reported to exert anti-atherosclerotic effects in pre-clinical model of disease. Reduction of plaque burden was associated with plaque stabilisation documented by the reduction in the content of macrophages, apoptotic cells, MMPs and endothelin-1, and the increase in smooth muscle cells content. TP-receptor blockade might have an anti-atherosclerotic and plaque stabilisation effect. The possibility of combining anti-platelet activity with an anti-atherosclerotic effect via selective TP-receptor inhibitors could have important implications especially in clinical conditions associated with increased production of prostanoids, such as diabetes.

    Citation

    Chiara Giannarelli, M Urooj Zafar, Juan J Badimon. Prostanoid and TP-receptors in atherothrombosis: is there a role for their antagonism? Thrombosis and haemostasis. 2010 Nov;104(5):949-54

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 20886180

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.