Global coagulation tests: their applicability for measuring direct factor Xa- and thrombin inhibition and reversal of anticoagulation by prothrombin complex concentrate
Research article published in Clinical chemistry and laboratory medicine (2014)
Abstract
BACKGROUND: Specific mass spectrometry and direct activated factor X (Xa)- and thrombin inhibition assays do not allow determination of the reversal of anticoagulant effects of non-vitamin K direct oral anticoagulants (NOACs) by prothrombin complex concentrate (PCC). The objective of this study was the evaluation of the applicability of a variety of commercially available global coagulation assays in analyzing the reversal of NOAC anticoagulation by PCC. METHODS: Plasma and whole blood were spiked with apixaban or dabigatran and PCC was added to these samples. Prothrombin time (PT), modified PT (mPT), activated partial prothrombin time (APTT), thrombography (CAT method) and thromboelastography (ROTEM, TEG) were performed. RESULTS: Assays triggered by contact activation (APTT, INTEM) did not show inhibitor reversal by PCC. Assays triggered by tissue factor (TF) showed NOAC type and NOAC concentration dependent anticoagulation reversal effects of PCC ranging from partial normalization to overcorrection of the following parameters: clotting or reaction time (PT, mPT TEG-TF, EXTEM, FIBTEM); angle in thromboelastography (TEG-TF); thrombin generation (CAT) lag time, endogenous thrombin potential (ETP) and peak thrombin. Extent of reversal was assay reagent dependent. ETP (5 pM TF) was the only parameter showing complete reversal of anticoagulation by PCC for all NOACs ranging from 200 to 800 μg/L. CONCLUSIONS: ETP fits with the concept that reversal assessment of NOAC anticoagulation by PCC should be based on measurements on the clotting potential or thrombin generating potential of the plasma or whole blood patient sample. Low sensitivity of ETP for NOACs and its correlation with bleeding are issues that remain to be resolved.
Abstract sourced from PubMed (NCBI) for the cited record. See the original publication for the authoritative version.
Summary
Peer-reviewed leech-derived compound and anticoagulant pharmacology relevant to medicinal leech therapy and its biology. Indexed in PubMed and verified against the NCBI record.
Why This Matters for Hirudotherapy
This laboratory study tested whether commercially available global coagulation assays can detect reversal of direct factor Xa and direct thrombin inhibitors (apixaban and dabigatran) by prothrombin complex concentrate (PCC) in spiked plasma and whole blood; the abstract reports that contact-activation assays (APTT, INTEM) showed no reversal, tissue-factor-triggered assays showed inhibitor-type- and concentration-dependent reversal, and that endogenous thrombin potential (ETP) was the only parameter showing complete reversal across all the direct oral anticoagulants tested. For hirudotherapy this is peripheral but instructive context on the laboratory monitoring of direct thrombin/Xa inhibition, the same enzymatic targets that the leech's hirudin and related secretome molecules act upon, and on the general difficulty of measuring and reversing direct anticoagulant effects. The honest caveat is that this is an in-vitro spiking study of synthetic anticoagulants and a reversal agent; it does not involve leeches, hirudin, or any clinical patient outcome, and the authors note open questions about ETP's sensitivity and its correlation with bleeding.
Citation
Global coagulation tests: their applicability for measuring direct factor Xa- and thrombin inhibition and reversal of anticoagulation by prothrombin complex concentrate.
Dinkelaar J et al. · Clinical chemistry and laboratory medicine, 2014
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