| Literature DB >> 33733989 |
Ramona Vinci1, Daniela Pedicino2, Alessia D'Aiello1, Pellegrino Ciampi1, Myriana Ponzo1, Alice Bonanni1, Giulio Russo1, Rocco Antonio Montone2, Massimo Massetti1,2, Filippo Crea1,2, Giovanna Liuzzo1,2.
Abstract
Acute Coronary Syndromes (ACS) with plaque erosion display dysregulated hyaluronan metabolism, with increased hyaluronidase-2 (HYAL2) expression. However, the expression and the role of this enzyme on platelets has never been explored. We evaluated the platelet's HYAL2 (pltHYAL2) levels on I) stable angina (SA) and II) ACS patients, furtherly sub-grouped in Intact-Fibrous-Cap (IFC) and Ruptured-Fibrous-Cap (RFC), according to Optical Coherence Tomography. We assessed the HYAL2 role through an in vitro model setting of co-cultured monocytes and platelets, before and after treatment with low-molecular-weight hyaluronic acid (HA) as pro-inflammatory stimulus and with or without HYAL2-antibody to inhibit HYAL2 activity. ACS patients exhibit higher pltHYAL2 levels comparing to SA, with the higher expression for IFC group. The addition of HYAL2-antibody significantly reduced the percentage of monocyte-platelet binding, suggesting that pltHYAL2 enrichment at the site of the culprit lesion is a key mediator in the systemic thrombo-inflammatory status of ACS presenting with plaque erosion.Entities:
Keywords: Acute coronary syndromes; hyaluronic acid; hyaluronidase; personalised medicine; platelets
Year: 2021 PMID: 33733989 PMCID: PMC7993372 DOI: 10.1080/14756366.2021.1900159
Source DB: PubMed Journal: J Enzyme Inhib Med Chem ISSN: 1475-6366 Impact factor: 5.051