Protease-activated receptors in vascular smooth muscle cells: a bridge between thrombo-inflammation and vascular remodelling

Anxhela Habibi*, Wolfram Ruf, Leon Schurgers

*Corresponding author for this work

Research output: Contribution to journal(Systematic) Review article peer-review

Abstract

Coagulation factors are responsible for blood clot formation yet have also non-canonical functions as signalling molecules. In this context, they can activate protease-activated receptors (PARs) ubiquitously expressed in the vasculature. During vascular repair, vascular smooth muscle cells (VSMCs) will switch from a contractile to a synthetic reparative phenotype. During prolonged vascular stress, VSMCs acquire a pathological phenotype leading to cardiovascular disease. Activated coagulation factors impact on vessel wall permeability and integrity after vascular injury with a key role for PAR activation on endothelial cells. The activation of PARs on VSMCs supports vessel wall repair following injury. Prolonged PAR activation, however, results in pathological vascular remodelling. Therefore, understanding the mechanisms of PAR activation on VSMCs is key to propel our understanding of the molecular and cellular mechanisms to develop novel therapeutic strategies to resolve vascular remodelling.In this review, we discuss recent advances on the role of PAR signalling on VSMCs and specifically their role in vascular remodelling contributing to cardiovascular disease. Additionally, we discuss current therapeutic strategies targeting PAR signalling - indirectly or directly - in relation to cardiovascular disease.
Original languageEnglish
Article number57
Number of pages17
JournalCell Communication and Signaling
Volume23
Issue number1
DOIs
Publication statusPublished - 31 Jan 2025

Keywords

  • Protease-activated receptors
  • VSMCs
  • Vascular remodelling
  • Thrombo-inflammation
  • Anticoagulants
  • TISSUE FACTOR
  • PROCOAGULANT ACTIVITY
  • ENDOTHELIAL-CELLS
  • NADPH OXIDASE
  • DABIGATRAN ETEXILATE
  • MOLECULAR-MECHANISMS
  • HUMAN PLATELETS
  • EXPRESSION
  • MIGRATION
  • GROWTH

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