Direct thrombin inhibitors, but not the direct factor Xa inhibitor rivaroxaban, increase tissue factor‐induced hypercoagulability in vitro and in vivo

Perzborn, Elisabeth; Heitmeier, Stefan; Buetehorn, Ulf; Laux, Volker

doi:10.1111/jth.12591

Cited by 59 publications

(46 citation statements)

References 26 publications

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“…The normalization of TG parameter values with those of reference plasmas did not affect results (not shown) . Our ex vivo findings reinforce those obtained in vitro using normal plasma spiked with rivaroxaban and 1‐picomolar to 20‐picomolar TF concentrations . Interestingly, we obtained PD mirror‐inverted time profiles to PK time profiles for both temporal parameters (lag time and time to peak), markedly for peak height and to a lesser extent for ETP, with peak height consistently more affected than ETP in agreement with previous findings .…”

Section: Discussionsupporting

confidence: 91%

Rivaroxaban pharmacodynamics in healthy volunteers evaluated with thrombin generation and the active protein C system: Modeling and assessing interindividual variability

Siguret

Abdoul

Delavenne

et al. 2019

Journal of Thrombosis and Haemostasis

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Background Rivaroxaban is a direct factor Xa inhibitor with substantial inter‐individual pharmacokinetic (PK) variability. Pharmacodynamic (PD) variability, especially assessed with thrombin generation (TG), has been less documented. Objectives (i) To assess TG parameter time profiles in healthy volunteers, with TG being studied under different conditions and (ii) to model the relationship between rivaroxaban concentrations and TG parameters and subsequently estimate interindividual variability. Methods Sixty healthy male volunteers (DRIVING‐NCT01627665) received a single 40‐mg rivaroxaban dose. Blood sampling was performed at baseline and 10 predefined time points over 24 h. The TG was investigated with the fully automated ST‐Genesia system (Stago), using two tissue‐factor (TF) concentrations, in the absence (−), or presence (+) of thrombomodulin (TM) for the lowest one. The PD models were built to characterize the relationships between plasma rivaroxaban concentrations and endogenous thrombin potential (ETP) or peak height induced by the lowest TF concentration. Results Thrombin generation parameter time profiles with the lowest TF concentration showed a good sensitivity to rivaroxaban, especially +TM (active protein C negative feedback). The relationship between rivaroxaban concentrations and TG parameters was modeled with a sigmoidal relation. Mean rivaroxaban concentrations halving the baseline value of ETP and peak height (−TM) (C50) were of 284 and 33.2 ng/mL, respectively: +TM, C50 declined to 19.4 and 13.8 ng/mL, reflecting a powerful inhibitory effect. The estimated C50 population coefficients of variation were of 12.2% (−TM) and 31.3% (+TM) with the peak height models, 34.8% (+TM) with the ETP model. Conclusions This low‐rivaroxaban to moderate‐rivaroxaban PD variability in healthy volunteers contrasts with the substantial PK variability and deserves to be studied in different patient settings.

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Section: Discussionsupporting

confidence: 91%

Rivaroxaban pharmacodynamics in healthy volunteers evaluated with thrombin generation and the active protein C system: Modeling and assessing interindividual variability

Siguret

Abdoul

Delavenne

et al. 2019

Journal of Thrombosis and Haemostasis

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“…This has been speculated to erroneously elevate ETP and peak values in the CAT® assay at thrombin inhibitor concentrations up to 200 nM (94 ng/ml) [35]. Yet, in a recent study using spiked plasma samples, prothrombin fragments F1 + 2 were also elevated [25]. In our study, ETP and peak values were elevated with increasing Dabi concentration ( Fig.…”

Section: Discussionmentioning

confidence: 52%

“…Previous reports on this have been inconsistent. Dabi has been shown to exert hypercoagulable effects at therapeutic concentrations [25][26][27], but some contradictory reports exist [19,23,24,28]. DTIs have been reported to inhibit thrombomodulin-mediated activation of protein C, and fibrinolysis at high concentrations of thrombomodulin [25,29,30].…”

Section: Discussionmentioning

confidence: 97%

From laboratory to clinical practice: Dabigatran effects on thrombin generation and coagulation in patient samples

Helin

Lemponen

Hjemdahl

et al. 2015

Thrombosis Research

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“…Several explanations have been proposed for the potential association between dabigatran and MI risk. Preclinical and clinical studies suggest that direct thrombin inhibitors might paradoxically enhance thrombin generation and might promote platelet activation [31,32]. On the contrary, warfarin reduces the risk of MI and it is therefore possible that dabigatran is less protective than warfarin against MI [33][34][35].…”

Section: Discussionmentioning

confidence: 99%

Acenocoumarol vs. low-dose dabigatran in real-world patients discharged after ischemic stroke

Τζιόμαλος

Giampatzis²,

Bouziana³

et al. 2016

Blood Coagulation &Amp; Fibrinolysis

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The aim of this study was to compare the efficacy of dabigatran 110 mg twice daily and acenocoumarol in patients with atrial fibrillation discharged after ischemic stroke. We prospectively studied 436 consecutive patients who were discharged after acute ischemic stroke (39.2% males, age 78.6 ± 6.7 years). Approximately 1 year after discharge, the functional status was assessed with the modified Rankin scale (mRS). Adverse outcome was defined as mRS between 2 and 6. The occurrence of ischemic stroke, myocardial infarction (MI) and death during the 1-year follow-up was also recorded. At discharge, 142 patients had atrial fibrillation. Acenocoumarol and dabigatran 110 mg twice daily were prescribed to 52.1 and 6.3% of these patients, respectively. At 1 year after discharge, there was a trend for patients treated with acenocoumarol to have lower mRS than patients prescribed dabigatran (2.3 ± 2.4 and 4.1 ± 2.2, respectively; P = 0.060). Adverse outcome rates and the incidence of stroke during follow-up did not differ between the two groups. The incidence of MI was almost three times higher in patients prescribed dabigatran than in those prescribed acenocoumarol, but this difference did not reach significance (11.1 and 4.0%, respectively; P = 0.254). The incidence of cardiovascular death was also almost three times higher in the former, but again this difference was not significant (33.3 and 12.2%, respectively; P = 0.237). In real-world patients with acute ischemic stroke, dabigatran 110 mg twice daily is as effective as acenocoumarol in preventing stroke but appears to be associated with worse long-term functional outcome and higher incidence of MI.

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Direct thrombin inhibitors, but not the direct factor Xa inhibitor rivaroxaban, increase tissue factor‐induced hypercoagulability in vitro and in vivo

Cited by 59 publications

References 26 publications

Rivaroxaban pharmacodynamics in healthy volunteers evaluated with thrombin generation and the active protein C system: Modeling and assessing interindividual variability

Rivaroxaban pharmacodynamics in healthy volunteers evaluated with thrombin generation and the active protein C system: Modeling and assessing interindividual variability

From laboratory to clinical practice: Dabigatran effects on thrombin generation and coagulation in patient samples

Acenocoumarol vs. low-dose dabigatran in real-world patients discharged after ischemic stroke

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