Plasma apixaban concentrations and thrombin generation assay parameters in response to dose reduction for atrial fibrillation

Author:

Yeo Muhan1ORCID,Lee So‐Ryoung12,Choi Eue‐Keun12ORCID,Choi JungMin2,Lee Kyung‐Yeon2,Ahn Hyo‐Jeong2,Kwon Soonil3,Park Hyoung‐Seob4,Kim Hyun Kyung5,Oh Seil12,Lip Gregory Y. H.167

Affiliation:

1. Department of Internal Medicine Seoul National University College of Medicine Seoul Republic of Korea

2. Department of Internal Medicine Seoul National University Hospital Seoul Republic of Korea

3. Department of Internal Medicine Seoul Metropolitan Government Seoul National University Boramae Medical Center Seoul Republic of Korea

4. Department of Internal Medicine Keimyung University Dongsan Medical Centre Daegu Republic of Korea

5. Department of Laboratory Medicine Seoul National University College of Medicine Seoul Republic of Korea

6. Liverpool Centre for Cardiovascular Science at University of Liverpool Liverpool John Moores University and Liverpool Chest and Heart Hospital Liverpool United Kingdom

7. Department of Clinical Medicine Aalborg University Aalborg Denmark

Abstract

AimsTo investigate plasma apixaban concentrations and thrombin generation assay (TGA) parameters across different apixaban doses in atrial fibrillation patients who had dose‐reduction criteria for apixaban.MethodsThis observational study included 374 patients (mean age 75.6 ± 7.7 years, 54.8% female) with dose‐reduction criteria for apixaban. The patients were divided into 3 groups: (i) on‐label standard dose (5 mg twice daily, n = 166); (ii) on‐label reduced dose (2.5 mg twice daily, n = 55); and (iii) off‐label underdose (2.5 mg twice daily, n = 153). Apixaban concentrations determined via the anti‐Xa assay and TGA parameters were compared at trough levels.ResultsThe off‐label underdose group exhibited significantly lower apixaban trough concentrations than the on‐label reduced‐dose and standard‐dose groups (56.7 ± 42.9 vs. 83.7 ± 70.4 vs. 129.9 ± 101.8 ng/mL, all P < .001). Less than 70% of all patients fell within the expected range of apixaban concentrations. Proportions exceeding the upper limit of the expected range were significantly lower in the off‐label underdose group (1.3%) than in the on‐label reduced‐dose (9.1%, P = .005) and standard‐dose (12.7%, P < .001) groups. The TGA parameters showed the on‐label standard‐dose group displaying the lowest thrombogenic profiles. Lower creatinine clearance was the most significant predictor of higher apixaban concentrations.ConclusionOff‐label underdosed apixaban resulted in lower apixaban concentrations than both on‐label standard and reduced‐dose regimens. A considerable proportion of the patients exhibited apixaban concentrations outside the expected range, suggesting the potential benefits of plasma concentration monitoring. Further studies are needed to compare dosages directly, investigate the impact of plasma apixaban concentration monitoring and validate the current dose‐reduction criteria.

Publisher

Wiley

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