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Myeloperoxidase induces the priming of platelets
- 1.0394796 - BFÚ 2014 RIV US eng J - Journal Article
Kolářová, Hana - Klinke, A. - Kremserová, Silvie - Adam, M. - Pekarová, Michaela - Baldus, S. - Eiserich, J.P. - Kubala, Lukáš
Myeloperoxidase induces the priming of platelets.
Free Radical Biology and Medicine. Roč. 61, AUG 2013 (2013), s. 357-369. ISSN 0891-5849. E-ISSN 1873-4596
R&D Projects: GA ČR(CZ) GCP305/12/J038
Institutional support: RVO:68081707
Keywords : ACUTE CORONARY SYNDROMES * NITRIC-OXIDE * REACTIVE OXYGEN
Subject RIV: BO - Biophysics
Impact factor: 5.710, year: 2013
The release of myeloperoxidase (MPO) from polymorphonuclear neutrophils is a hallmark of vascular inflammation and contributes to the pathogenesis of vascular inflammatory processes. However, the effects of MPO on platelets as a contributory mechanism in vascular inflammatory diseases remain unknown. Thus, MPO interaction with platelets and its effects on platelet function were examined. First, dose-dependent binding of MPO (between 1.7 and 13.8 nM) to both human and mouse platelets was observed. This was in direct contrast to the absence of MPO in megakaryocytes. MPO was localized both on the surface of and inside platelets. Cytoskeleton inhibition did not prevent MPO localization inside the three-dimensional platelet structure. MPO peroxidase activity was preserved upon the MPO binding to platelets. MPO sequestered in platelets catabolized NO, documented by the decreased production of NO (on average, an approximately 2-fold decrease). MPO treatment did not affect the viability of platelets during short incubations; however, it decreased platelet viability after long-term storage for 7 days (an approximately 2-fold decrease).
Permanent Link: http://hdl.handle.net/11104/0222966
Number of the records: 1