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Rivaroxaban, in combination with low-dose aspirin, is associated with a reduction in proinflammatory and prothrombotic circulating vesicle signatures in patients with cardiovascular disease

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Autor
Weiss, Luisa
O'Doherty, Aideen
Uhrig, Wido
Szklanna, Paulina B.
Hong-Minh, Molly
Wynne, Kieran
Blanco, Alfonso
Živný, JanORCiD Profile - 0000-0002-1811-8977WoS Profile - C-2545-2008Scopus Profile - 35265557200
Passos, Valeria Lima
Kevane, Barry
Murphy, Sean
Ainle, Fionnuala Ni
O'Donnell, Martin
Maguire, Patricia B.

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Datum vydání
2025
Publikováno v
Journal of Thrombosis and Haemostasis
Ročník / Číslo vydání
23 (2)
ISBN / ISSN
ISSN: 1538-7933
ISBN / ISSN
eISSN: 1538-7836
Informace o financování
MSM//LX22NPO5104
Metadata
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Kolekce
  • 1. lékařská fakulta

Tato publikace má vydavatelskou verzi s DOI 10.1016/j.jtha.2024.09.030

Abstrakt
Background: Despite secondary prevention with aspirin, patients with stable cardiovascular disease (CVD) remain at elevated long-term risk of major adverse cardiovascular events. The Cardiovascular Outcomes in People Using Anticoagulant Strategies (COMPASS) double-blind, randomized clinical trial demonstrated that aspirin plus low-dose rivaroxaban (COMPASS regime) significantly decreased the incidence of major adverse cardiovascular events by 24% compared with aspirin alone. However, the mechanisms underlying these potential synergistic/nonantithrombotic effects remain elusive. Extracellular vesicles (EVs) are crucial messengers regulating a myriad of biological/pathological processes and are highly implicated in CVD. Objectives: We hypothesized that circulating EV profiles reflect the cardioprotective properties of the COMPASS regime. Methods: A cohort of stable CVD patients (N = 40) who participated in the COMPASS trial and were previously randomized to receive aspirin were prospectively recruited and assigned a revised regimen of open-label aspirin plus rivaroxaban. Blood samples were obtained at baseline (aspirin only) and 6-month follow-up. Plasma EV concentration, size, and origin were analyzed by nanoparticle tracking analysis and flow cytometry. EVs were enriched by ultracentrifugation for proteomic analysis. Results: The COMPASS regime fundamentally altered small (<200 nm) and large (2001000 nm) EV concentration and size compared with aspirin alone. Crucially, levels of platelet-derived and myeloperoxidase-positive EVs became significantly decreased at follow-up. Comparative proteomic characterization further revealed a significant decrease in highly proinflammatory protein expression at follow-up. Conclusion: The observed changes in EV subpopulations, together with the differential protein expression profiles, suggest amelioration of an underlying proinflammatory and prothrombotic state upon dual therapy, which may be of clinical relevance toward understanding the fundamental mechanism underlying the reported superior cardiovascular outcomes associated with this antithrombotic regimen.
Klíčová slova
aspirin, cardiovascular disease, extracellular vesicles, proteomics, rivaroxaban,
Trvalý odkaz
https://hdl.handle.net/20.500.14178/3389
Zobraz publikaci v dalších systémech
WOS:001422467000001
SCOPUS:2-s2.0-85207763449
PUBMED:39413927
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