| Literature DB >> 32932519 |
Reiner K Mailer1, Mikel Allende1,2, Marco Heestermans1, Michaela Schweizer3, Carsten Deppermann1, Maike Frye1, Giordano Pula1, Jacob Odeberg4, Mathias Gelderblom5, Stefan Rose-John6, Albert Sickmann7, Stefan Blankenberg8, Tobias B Huber9, Christian Kubisch10, Coen Maas11, Stepan Gambaryan12, Dmitri Firsov13, Evi X Stavrou14,15, Lynn M Butler1,4, Thomas Renné1.
Abstract
Polyphosphate is a procoagulant inorganic polymer of linear-linked orthophosphate residues. Multiple investigations have established the importance of platelet polyphosphate in blood coagulation; however, the mechanistic details of polyphosphate homeostasis in mammalian species remain largely undefined. In this study, xenotropic and polytropic retrovirus receptor 1 (XPR1) regulated polyphosphate in platelets and was implicated in thrombosis in vivo. We used bioinformatic analyses of omics data to identify XPR1 as a major phosphate transporter in platelets. XPR1 messenger RNA and protein expression inversely correlated with intracellular polyphosphate content and release. Pharmacological interference with XPR1 activity increased polyphosphate stores, led to enhanced platelet-driven coagulation, and amplified thrombus formation under flow via the polyphosphate/factor XII pathway. Conditional gene deletion of Xpr1 in platelets resulted in polyphosphate accumulation, accelerated arterial thrombosis, and augmented activated platelet-driven pulmonary embolism without increasing bleeding in mice. These data identify platelet XPR1 as an integral regulator of platelet polyphosphate metabolism and reveal a fundamental role for phosphate homeostasis in thrombosis.Entities:
Year: 2021 PMID: 32932519 PMCID: PMC7955403 DOI: 10.1182/blood.2019004617
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113