| Literature DB >> 27436851 |
Kate Burley1, Claire S Whyte2, Sarah K Westbury1, Mary Walker3, Kathleen E Stirrups4,5, Ernest Turro4,5,6, Oliver G Chapman7, Christopher Reilly-Stitt3, Nicola J Mutch2, Andrew D Mumford1.
Abstract
Thrombomodulin-associated coagulopathy (TM-AC) is a newly recognized dominant bleeding disorder in which a p.Cys537Stop variant in the thrombomodulin (TM) gene THBD, results in high plasma TM levels and protein C-mediated suppression of thrombin generation. Thrombin in complex with TM also activates thrombin-activatable fibrinolysis inhibitor (TAFI). However, the effect of the high plasma TM on fibrinolysis in TM-AC is unknown. Plasma from TM-AC cases and high-TM model control samples spiked with recombinant soluble TM showed reduced tissue factor-induced thrombin generation. Lysis of plasma clots from TM-AC cases was significantly delayed compared with controls but was completely restored when TM/thrombin-mediated TAFI activation was inhibited. Clots formed in blood from TM-AC cases had the same viscoelastic strength as controls but also showed a TAFI-dependent delay in fibrinolysis. Delayed fibrinolysis was reproduced in high-TM model plasma and blood samples. Partial restoration of thrombin generation with recombinant activated factor VII or activated prothrombin complex concentrate did not alter the delayed fibrinolysis in high-TM model blood. Our finding of a previously unrecognized fibrinolytic phenotype indicates that bleeding in TM-AC has a complex pathogenesis and highlights the pivotal role of TM as a regulator of hemostasis.Entities:
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Year: 2016 PMID: 27436851 PMCID: PMC5054699 DOI: 10.1182/blood-2016-05-716092
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113