Pharmacokinetic and pharmacodynamic effects of comedication of clopidogrel and dabigatran etexilate in healthy male volunteers

Härtter, Sebastian; Sennewald, Regina; Schepers, Cornelia; Baumann, Sybille; Fritsch, Holger; Friedman, Jeffrey

doi:10.1007/s00228-012-1304-8

Cited by 22 publications

(26 citation statements)

References 25 publications

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“…While brief descriptions of plasma dabigatran assays have been reported in several clinical papers , only Delavenne et al . have published a comprehensive dabigatran assay method detailing the development and validation procedures in accordance with FDA guidelines .…”

Section: Measuring Dabigatran Concentrationsmentioning

confidence: 99%

“…Reports of the contribution of the dabigatran glucuronides to total active drug‐related exposure in plasma from dabigatran etexilate range from 10 to 35% , with no apparent influence of mild to severe renal or moderate hepatic impairment . The range is only slightly narrower (15–35%) when the reports are restricted to those involving healthy young individuals who were administered a single dabigatran etexilate dose of 150 mg . However, the variability of the contribution of the glucuronides to overall drug exposure has been reported to be low in healthy young individuals, as reflected by a coefficient of variation (CV) of 8–10% .…”

Section: Measuring Dabigatran Concentrationsmentioning

confidence: 99%

“…For example, the glucuronides may be unstable during sample storage . This is difficult to establish as the glucuronides were not assayed directly in any of the reported studies . Instead, these were inferred from the difference in plasma dabigatran concentrations before and after alkalinization (hydrolyzing the glucuronides to dabigatran) .…”

Section: Measuring Dabigatran Concentrationsmentioning

confidence: 99%

“…Other P‐glycoprotein inhibitors (with reported mean AUC(0,∞) ratio) include: ketoconazole (2.5) ; dronedarone (2.0) ; amiodarone (1.6) ; clarithromycin (1.5) ; quinidine (1.5) ; ticagrelor (1.5) [72] loading doses of clopidogrel (1.3) .…”

Section: The Thrombin Time For Monitoring Dabigatran Effect and Guidimentioning

confidence: 99%

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A proposal for dose‐adjustment of dabigatran etexilate in atrial fibrillation guided by thrombin time

Chin

Wright

Patterson

et al. 2014

Brit J Clinical Pharma

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Dabigatran is an oral anticoagulant that is increasingly used for atrial fibrillation (AF). Presently, many authorities state that routine laboratory coagulation monitoring is not required. However, data have recently been published demonstrating that higher trough plasma dabigatran concentrations are associated with lower thromboembolic and higher haemorrhagic event rates. Using these data, we simulate a range of AF patients with varying risks for these events and derive a target range of trough plasma dabigatran concentrations (30-130 μg l −1). Finally, we propose that a conventional screening coagulation assay, the thrombin time (TT), can be used to discern whether or not patients are within this range of dabigatran concentrations.

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Section: Measuring Dabigatran Concentrationsmentioning

confidence: 99%

Section: Measuring Dabigatran Concentrationsmentioning

confidence: 99%

Section: Measuring Dabigatran Concentrationsmentioning

confidence: 99%

Section: The Thrombin Time For Monitoring Dabigatran Effect and Guidimentioning

confidence: 99%

See 2 more Smart Citations

A proposal for dose‐adjustment of dabigatran etexilate in atrial fibrillation guided by thrombin time

Chin

Wright

Patterson

et al. 2014

Brit J Clinical Pharma

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“…Dabigatran and clopidogrel had no clinically relevant pharmacokinetic or pharmacodynamic effects on each other. However, if a loading dose of clopidogrel (300 mg or 600 mg) was administered, dabigatran AUC and C max at steady state increased by 30–40% . For drug interactions with P‐gp inducers and inhibitors, the maximum increase in dabigatran bioavailability was observed with ketoconazole (~150%) .…”

Section: Mechanism Of Action and Clinical Pharmacologymentioning

confidence: 99%

Non-vitamin K antagonist oral anticoagulants in cardiovascular disease management: evidence and unanswered questions

Cheng

Barillari

2014

J Clin Pharm Ther

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Summary What is known and objective Anticoagulation is important in the management of cardiovascular disorders; however, traditional anticoagulants such as heparins and vitamin K antagonists (VKAs) have limitations, including parenteral administration with the former and the need for coagulation monitoring and dose adjustments with the latter. Three non‐VKA oral anticoagulants (OACs), dabigatran, rivaroxaban and apixaban, are available for the prevention of stroke in patients with atrial fibrillation (AF) and may change clinical practice. This article reviews current knowledge and important unanswered questions on the use of these agents in patients with cardiovascular disease. Methods A literature search was performed using PubMed and the search terms dabigatran, rivaroxaban, apixaban, AF and acute coronary syndrome (ACS). Peer‐reviewed, published clinical trials, review articles, relevant treatment guidelines and prescribing information documents were identified and reviewed for relevance. Results and discussion Dabigatran is an oral direct thrombin inhibitor; rivaroxaban and apixaban are oral direct Factor Xa inhibitors. These agents have a quicker onset and offset of action, more predictable pharmacokinetic and pharmacodynamic profiles, and fewer drug–drug interactions than VKAs, allowing use of fixed doses. For the prevention of stroke in patients with AF, the non‐VKA OACs were either non‐inferior or superior to warfarin with similar or improved bleeding profiles, particularly with respect to reductions in intracranial haemorrhage. In patients with ACS receiving dual antiplatelet therapy, the addition of rivaroxaban significantly reduced the rate of death from cardiovascular causes, myocardial infarction or stroke without increasing fatal bleeding, but led to higher rates of major bleeding. Dose reductions with non‐VKA OACs are mandated in certain circumstances in patients with AF, such as moderate renal impairment. Contraindications include creatinine clearance <15 mL/min (<30 mL/min for dabigatran in Europe and Canada) and moderate or severe hepatic impairment, but patients can be transitioned to other anticoagulants if appropriate. It is unknown which non‐VKA OAC is optimal for stroke prevention in patients with AF, although factors such as co‐medications (e.g. dabigatran may be preferred if a patient is taking a co‐medication that is a strong cytochrome P450 3A4 inhibitor) and renal function (rivaroxaban and apixaban depend less on renal clearance than dabigatran) will be important for individual patients. Addition of rivaroxaban to antiplatelet therapy for prevention of recurrent events in patients with recent ACS is approved in Europe for patients at the highest risk (with elevated cardiac biomarkers) and must take into account the increased risk of major bleeding. Although routine coagulation monitoring is not required, an understanding of which assays are appropriate for each non‐VKA OAC and how they are affected is important. In a bleeding emergency, non‐specific prohaemostatic agents are suggested ...

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Investigation of the Effect of Lasmiditan on the Pharmacokinetics of P‐Glycoprotein and Breast Cancer Resistance Protein Substrates

Luffer‐Atlas,

Wilbraham,

Posada

et al. 2023

The Journal of Clinical Pharma

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Lasmiditan is an in vitro inhibitor of P‐glycoprotein (P‐gp) and breast cancer resistance protein (BCRP) efflux transporters. We aimed to confirm predictions from physiologically‐based pharmacokinetic models of lasmiditan and assess the safety and tolerability of rosuvastatin and dabigatran co‐administered with lasmiditan. In this open‐label, post‐marketing drug‐drug interaction phase 1 clinical trial, eligible participants were adults 21–70 years old with body mass index 18.5–35.0 kg/m2. Part 1 (P‐gp: 150 mg dabigatran etexilate with 200 mg lasmiditan) and Part 2 (BCRP: 10 mg rosuvastatin with 200 mg lasmiditan) employed similar designs: single dose of probe substrate administered Day −2 with pharmacokinetic evaluation; 1‐week washout; lasmiditan administered Days 8 and 9 alone; lasmiditan co‐administered with single dose of probe substrate Day 10 with pharmacokinetic evaluation of probe substrate and lasmiditan. Sixty‐six participants were included in Part 1 and 30 in Part 2. Following dabigatran co‐administration with lasmiditan vs. dabigatran alone, 90% confidence intervals for geometric least squares (LS) mean ratios of AUC[0‐∞] and Cmax were not contained within non‐effect boundaries (0.80–1.25). Dabigatran AUC[0‐∞] increased by 25% and Cmax by 22%. Median tmax for dabigatran was 2.0–3.0 hours. Following rosuvastatin co‐administration with lasmiditan vs. rosuvastatin alone, 90% CIs for geometric LS mean ratios of AUC[0‐∞] and Cmax were contained within non‐effect boundaries (0.80–1.25). Rosuvastatin AUC[0‐∞] increased by 15% and Cmax by 7%. Median tmax for rosuvastatin was 4.0 hours. Results suggest that lasmiditan has a weak effect on P‐gp substrates and no clinically relevant effect on BCRP substrates.This article is protected by copyright. All rights reserved

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Pharmacokinetic and pharmacodynamic effects of comedication of clopidogrel and dabigatran etexilate in healthy male volunteers

Cited by 22 publications

References 25 publications

A proposal for dose‐adjustment of dabigatran etexilate in atrial fibrillation guided by thrombin time

A proposal for dose‐adjustment of dabigatran etexilate in atrial fibrillation guided by thrombin time

Non-vitamin K antagonist oral anticoagulants in cardiovascular disease management: evidence and unanswered questions

Investigation of the Effect of Lasmiditan on the Pharmacokinetics of P‐Glycoprotein and Breast Cancer Resistance Protein Substrates

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