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RSS FeedsIJMS, Vol. 20, Pages 5629: Using PAR4 Inhibition as an Anti-Thrombotic Approach: Why, How, and When? (International Journal of Molecular Sciences)

 
 

11 november 2019 15:02:29

 
IJMS, Vol. 20, Pages 5629: Using PAR4 Inhibition as an Anti-Thrombotic Approach: Why, How, and When? (International Journal of Molecular Sciences)
 


Protease-activated receptors (PARs) are a family of four GPCRs with a variety of cellular functions, yet the only advanced clinical endeavours to target these receptors for therapeutic gain to date relates to the impairment of platelet function for anti-thrombotic therapy. The only approved PAR antagonist is the PAR1 inhibitor, vorapaxar—the sole anti-platelet drug against a new target approved in the past 20 years. However, there are two PARs on human platelets, PAR1 and PAR4, and more recent efforts have focused on the development of the first PAR4 antagonists, with first-in-class agents recently beginning clinical trial. Here, we review the rationale for this approach, outline the various modes of PAR4 inhibition, and speculate on the specific therapeutic potential of targeting PAR4 for the prevention of thrombotic conditions.


 
214 viewsCategory: Biochemistry, Biophysics, Molecular Biology
 
IJMS, Vol. 20, Pages 5631: The Bile Acid-Phospholipid Conjugate Ursodeoxycholyl-Lysophosphatidylethanolamide (UDCA-LPE) Disintegrates the Lipid Backbone of Raft Plasma Membrane Domains by the Removal of the Membrane Phospholipase A2 (International Journal of Molecular Sciences)
IJMS, Vol. 20, Pages 5628: RgsA Attenuates the PKA Signaling, Stress Response, and Virulence in the Human Opportunistic Pathogen Aspergillus fumigatus (International Journal of Molecular Sciences)
 
 
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