Comparison of the pharmacokinetics and pharmacodynamics of apixaban and rivaroxaban in dogs

Background Comparative pharmacokinetics and pharmacodynamics (PK/PD) of apixaban and rivaroxaban have not been studied in dogs and the propensity of these drugs to cause hypercoagulability after discontinuation is unknown. Hypothesis Compare the PK/PD of clinical dosing regimens of PO apixaban and r...

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Published in:Journal of veterinary internal medicine 2024-11, Vol.38 (6), p.3242-3254
Main Authors: Lynch, Alex M., Ruterbories, Laura K., Zhu, Yao, Fialkiewicz, Frank, Papich, Mark G., Brooks, Marjory B., Goggs, Robert
Format: Article
Language:English
Subjects:
Animals
anticoagulant
Anticoagulants
Anticoagulants - administration & dosage
Anticoagulants - pharmacokinetics
Anticoagulants - pharmacology
anti‐Xa
Biological activity
Blood Coagulation - drug effects
Calibration
Chromatography
direct oral anticoagulant
DOAC
Dogs
Drug dosages
Factor Xa Inhibitors - pharmacokinetics
Factor Xa Inhibitors - pharmacology
Female
Laboratory animals
Male
Mass spectrometry
Pharmacodynamics
Pharmacokinetics
Phlebotomy
Plasma
Pyrazoles - blood
Pyrazoles - pharmacokinetics
Pyrazoles - pharmacology
Pyridones - administration & dosage
Pyridones - blood
Pyridones - pharmacokinetics
Pyridones - pharmacology
Quality control
Rivaroxaban - pharmacokinetics
Rivaroxaban - pharmacology
Scientific imaging
SMALL ANIMAL
thrombin generation
Thromboembolism
thromboprophylaxis
Thrombosis
Veterinary medicine
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Summary:Background Comparative pharmacokinetics and pharmacodynamics (PK/PD) of apixaban and rivaroxaban have not been studied in dogs and the propensity of these drugs to cause hypercoagulability after discontinuation is unknown. Hypothesis Compare the PK/PD of clinical dosing regimens of PO apixaban and rivaroxaban administered repeatedly to healthy dogs and assess the effect of abrupt drug discontinuation on coagulation. Animals Six University‐owned, purpose‐bred, middle‐aged, mixed‐breed dogs (4 male, 2 female). Methods Dogs were given apixaban or rivaroxaban PO at 0.5 mg/kg q12h for 7 days with a 14‐day washout period between drugs. Plasma drug concentrations were quantitated, and anticoagulant effects were measured using clotting times, calibrated anti‐Xa bioactivity assays, and measurements of thrombin generation. The potential for rebound hypercoagulability was assessed by measuring D‐dimers, thrombin‐antithrombin (TAT) complexes, and antithrombin activity after drug discontinuation. Results Plasma drug concentrations and anti‐Xa bioactivities were closely correlated for both drugs, but drug concentrations varied considerably among dogs, despite consistent dose regimens. Thrombin generation variables were significantly correlated with the anti‐Xa bioactivity of both drugs and no significant differences in the effects of apixaban and rivaroxaban on thrombin generation were observed. Drug discontinuation had no effect on D‐dimer concentrations. The concentration of TAT complexes decreased after apixaban discontinuation and did not change after rivaroxaban discontinuation. Conclusions and Clinical Importance Repeated PO administration of apixaban or rivaroxaban to healthy dogs produced comparable anticoagulant effects measured by inhibition of thrombin formation. Rebound hypercoagulability after drug discontinuation was not observed and weaning of these drugs in clinical patients might not be necessary.
ISSN:0891-6640
1939-1676
1939-1676
DOI:10.1111/jvim.17216