Literature DB >> 14529396

Development of proteinase-activated receptor 1 antagonists as therapeutic agents for thrombosis, restenosis and inflammatory diseases.

Ho-Sam Ahn1, Samuel Chackalamannil, George Boykow, Michael P Graziano, Carolyn Foster.   

Abstract

Thrombin, a plasma serine protease, plays a key role not only in coagulation and hemostasis but in thrombosis, restenosis and atherosclerosis. Thrombin activates platelets, endothelium, inflammatory cells and smooth muscle cells. The cellular action of thrombin is mediated by specific G-protein coupled thrombin receptors called proteinase-activated receptors (protease-activated receptor or PARs). Among the three thrombin receptors, PAR1 is the primary thrombin receptor in human and animal cells with an exception of non-primate platelets. An increased thrombin generation and PAR1 expression are observed on cells within atherosclerotic plaque and thrombus and following vascular injury. Animal studies with PAR1 deficient mice and small molecule antagonists indicate an important role of PAR1 in thrombosis and restenosis and thus the therapeutic potential of a PAR1 antagonist in treating these diseases. Development of a thrombin receptor tethered ligand analog binding assay led to the discovery of several different series of potent, nonpeptide small molecular antagonists of PAR1. These antagonists are PAR1 selective and inhibit most of the cellular effects of thrombin. A PAR1 antagonist has an advantage over a direct thrombin inhibitor since it does not inhibit enzymatic action of thrombin in the coagulation cascade with the consequent minimal bleeding side-effects, unlike a direct thrombin inhibitor. In addition, the emerging evidence for the role of PAR1 in various inflammatory diseases suggests as yet unexplored therapeutic potentials of PAR1 antagonists in various inflammatory diseases.

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Year:  2003        PMID: 14529396     DOI: 10.2174/1381612033453884

Source DB:  PubMed          Journal:  Curr Pharm Des        ISSN: 1381-6128            Impact factor:   3.116


  13 in total

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2.  Selecting optimal antiplatelet therapy based on platelet function monitoring in patients with coronary artery disease.

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Review 4.  Thrombin and vascular inflammation.

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Journal:  Mol Cell Biochem       Date:  2011-08-23       Impact factor: 3.396

Review 5.  Pregnancy-specific expression of protease-activated receptor 1: a therapeutic target for prevention and treatment of preeclampsia?

Authors:  Scott W Walsh; Jerome F Strauss
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Journal:  PLoS One       Date:  2009-12-21       Impact factor: 3.240

7.  Protease Amplification of the Inflammatory Response Induced by Commensal Bacteria: Implications for Racial Disparity in Term and Preterm Birth.

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Journal:  Reprod Sci       Date:  2020-01-01       Impact factor: 3.060

8.  Proteases Activate Pregnancy Neutrophils by a Protease-Activated Receptor 1 Pathway: Epigenetic Implications for Preeclampsia.

Authors:  Scott W Walsh; William H Nugent; Marwah Al Dulaimi; Sonya L Washington; Phoebe Dacha; Jerome F Strauss
Journal:  Reprod Sci       Date:  2020-06-15       Impact factor: 3.060

9.  Novel role for p21-activated kinase 2 in thrombin-induced monocyte migration.

Authors:  Ravisekhar Gadepalli; Sivareddy Kotla; Mark R Heckle; Shailendra K Verma; Nikhlesh K Singh; Gadiparthi N Rao
Journal:  J Biol Chem       Date:  2013-09-11       Impact factor: 5.157

Review 10.  The Road to Low-Dose Aspirin Therapy for the Prevention of Preeclampsia Began with the Placenta.

Authors:  Scott W Walsh; Jerome F Strauss
Journal:  Int J Mol Sci       Date:  2021-06-29       Impact factor: 5.923

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