Platelet olfactory receptor activation limits platelet reactivity and growth of aortic aneurysms

  • Craig N. Morrell
  • , Doran Mix
  • , Anu Aggarwal
  • , Rohan Bhandari
  • , Matthew Godwin
  • , Phillip Owens
  • , Sean P. Lyden
  • , Adam Doyle
  • , Krystin Krauel
  • , Matthew T. Rondina
  • , Amy Mohan
  • , Charles J. Lowenstein
  • , Sharon Shim
  • , Shaun Stauffer
  • , Vara Prasad Josyula
  • , Sara K. Ture
  • , David I. Yule
  • , Larry E. Wagner
  • , John M. Ashton
  • , Ayman Elbadawi
  • Scott J. Cameron

Research output: Contribution to journalArticlepeer-review

34 Scopus citations

Abstract

As blood transitions from steady laminar flow (S-flow) in healthy arteries to disturbed flow (D-flow) in aneurysmal arteries, platelets are subjected to external forces. Biomechanical platelet activation is incompletely understood and is a potential mechanism behind antiplatelet medication resistance. Although it has been demonstrated that antiplatelet drugs suppress the growth of abdominal aortic aneurysms (AAA) in patients, we found that a certain degree of platelet reactivity persisted in spite of aspirin therapy, urging us to consider additional antiplatelet therapeutic targets. Transcriptomic profiling of platelets from patients with AAA revealed upregulation of a signal transduction pathway common to olfactory receptors, and this was explored as a mediator of AAA progression. Healthy platelets subjected to D-flow ex vivo, platelets from patients with AAA, and platelets in murine models of AAA demonstrated increased membrane olfactory receptor 2L13 (OR2L13) expression. A drug screen identified a molecule activating platelet OR2L13, which limited both biochemical and biomechanical platelet activation as well as AAA growth. This observation was further supported by selective deletion of the OR2L13 ortholog in a murine model of AAA that accelerated aortic aneurysm growth and rupture. These studies revealed that olfactory receptors regulate platelet activation in AAA and aneurysmal progression through platelet-derived mediators of aortic remodeling.

Original languageEnglish (US)
Article numbere152373
JournalJournal of Clinical Investigation
Volume132
Issue number9
DOIs
StatePublished - May 2 2022

ASJC Scopus subject areas

  • General Medicine

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