A study of endothelial and platelet microvesicles across different hypertension phenotypes. 2022

Antonios Lazaridis, and Eleni Gavriilaki, and Barbara Nikolaidou, and Efi Yiannaki, and Panagiotis Dolgyras, and Panagiota Anyfanti, and Areti Triantafyllou, and Nikolaos Koletsos, and Christos Tzimos, and Dimitra Markala, and Stella Douma, and Eugenia Gkaliagkousi
3rd Department of Internal Medicine, Papageorgiou Hospital, Aristotle University of Thessaloniki, Thessaloniki, Greece.

Rather than being mere biomarkers reflecting generalized vascular injury, endothelial- (EMVs) and platelet-derived (PMVs) microvesicles have emerged as potent regulators of intercellular communication with significant biologic effects in vascular homeostasis and several pathophysiological responses including inflammation and thrombosis. So far, studies in hypertension are scarce, whereas no studies exist in masked hypertension (MH). We measured EMVs and PMVs in untreated, newly diagnosed hypertensives (HTs) and MHs compared to normotensive controls (NTs), and associated them with various cardiovascular risk factors. Sustained hypertension (SHT) and MH were defined according to standard blood pressure (BP) criteria. All HTs were free of cardiovascular disease and medications. Microvesicles' quantitation and detection were performed by flow cytometry by using cell-specific antibodies and corresponding isotypes (anti-CD105 and anti-CD144 for EMVs, anti-CD42a for PMVs, and Annexin V-fluorescein isothiocyanate for all microvesicles). In this study, we included 59 HTs (44 SHTs and 15 MHs) and 27 NTs. HTs had significantly elevated EMVs (p = 0.004), but not PMVs compared to NTs. MHs had significantly elevated EMVs compared to NTs (p = 0.012) but not compared to SHTs. Furthermore, EMVs significantly correlated with ambulatory (r = 0.214-0.284), central BP (r = 0.247-0.262), and total vascular resistance (r = 0.327-0.361). EMVs are increased not only in SHTs but also in MHs, a hypertension phenotype with a cardiovascular risk close to SHT. EMVs have emerged as active contributors to thromboinflammation and vascular damage and may explain, in part, the adverse cardiovascular profile of SHTs and MHs.

UI MeSH Term Description Entries
D006973 Hypertension Persistently high systemic arterial BLOOD PRESSURE. Based on multiple readings (BLOOD PRESSURE DETERMINATION), hypertension is currently defined as when SYSTOLIC PRESSURE is consistently greater than 140 mm Hg or when DIASTOLIC PRESSURE is consistently 90 mm Hg or more. Blood Pressure, High,Blood Pressures, High,High Blood Pressure,High Blood Pressures
D007249 Inflammation A pathological process characterized by injury or destruction of tissues caused by a variety of cytologic and chemical reactions. It is usually manifested by typical signs of pain, heat, redness, swelling, and loss of function. Innate Inflammatory Response,Inflammations,Inflammatory Response, Innate,Innate Inflammatory Responses
D010641 Phenotype The outward appearance of the individual. It is the product of interactions between genes, and between the GENOTYPE and the environment. Phenotypes
D006801 Humans Members of the species Homo sapiens. Homo sapiens,Man (Taxonomy),Human,Man, Modern,Modern Man
D013927 Thrombosis Formation and development of a thrombus or blood clot in BLOOD VESSELS. Atherothrombosis,Thrombus,Blood Clot,Blood Clots,Thromboses
D055252 Cell-Derived Microparticles Extracellular vesicles generated by the shedding of CELL MEMBRANE blebs. Cell Membrane Microparticles,Circulating Cell-Derived Microparticles,Ectosomes,Microparticles, Cell-Derived,Shedding Microvesicles,Cell Derived Microparticles,Cell Membrane Microparticle,Cell-Derived Microparticle,Cell-Derived Microparticle, Circulating,Cell-Derived Microparticles, Circulating,Circulating Cell Derived Microparticles,Circulating Cell-Derived Microparticle,Ectosome,Membrane Microparticle, Cell,Membrane Microparticles, Cell,Microparticle, Cell Membrane,Microparticle, Cell-Derived,Microparticle, Circulating Cell-Derived,Microparticles, Cell Derived,Microparticles, Cell Membrane,Microparticles, Circulating Cell-Derived,Microvesicle, Shedding,Microvesicles, Shedding,Shedding Microvesicle

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