Assessing Potential Drug–Drug Interactions Between Dabigatran Etexilate and a P‐Glycoprotein Inhibitor in Renal Impairment Populations Using Physiologically Based Pharmacokinetic Modeling

Doki, Kosuke; Rostami‐Hodjegan, Amin; Homma, Masato

doi:10.1002/psp4.12382

Cited by 17 publications

(17 citation statements)

References 25 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…A combination of increased absorption and reduced elimination can also lead to increased DOAC exposure that has previously not been investigated. A physiologically based pharmacokinetic model calculated that dabigatran C min will significantly increase in patients with moderate renal impairment who concomitantly take the P-gp inhibitor verapamil [72]. Despite the statement in the product label that only recommends a dose reduction to 110 mg twice daily, the authors suggested that the significantly increased C min values might be preventable by reducing dabigatran doses further to 75 mg twice daily [72].…”

Section: Drug-drug Interactions Affecting Doac Therapymentioning

confidence: 99%

“…A physiologically based pharmacokinetic model calculated that dabigatran C min will significantly increase in patients with moderate renal impairment who concomitantly take the P-gp inhibitor verapamil [72]. Despite the statement in the product label that only recommends a dose reduction to 110 mg twice daily, the authors suggested that the significantly increased C min values might be preventable by reducing dabigatran doses further to 75 mg twice daily [72]. However, as long as clinical trials investigating pharmacokinetics and clinical effects of this complex clinical situation are missing, it will be unclear whether patients treated with 110 mg twice daily are at an increased risk of bleeding and what dabigatran efficacy will be if doses are further reduced.…”

Section: Drug-drug Interactions Affecting Doac Therapymentioning

confidence: 99%

See 1 more Smart Citation

Drug–Drug Interactions with Direct Oral Anticoagulants

et al. 2020

View full text Add to dashboard Cite

A large body of evidence suggests that not only direct anticoagulant effects but also major bleeding events and stroke prevention depend on plasma concentrations of direct oral anticoagulants (DOACs). Concomitant drugs that cause drug-drug interactions (DDIs) alter DOAC exposure by increasing or decreasing DOAC bioavailability and/or clearance; hence, they might affect the efficacy and safety of DOAC therapy. Patients with renal impairment already receive smaller DOAC maintenance doses because avoidance of elevated DOAC exposure might prevent serious bleeding events. For other causes of increased exposure such as DDIs, management is often less well-defined. Considering that DOAC patients are often older and have multiple co-morbidities, polypharmacy is highly prevalent. However, the effect of multiple drugs on DOAC exposure, and especially the impact of DDIs when concurring with drug-disease interactions as observed in renal impairment, has not been thoroughly elucidated. In order to provide effective and safe anticoagulation with DOACs, understanding the mechanisms and magnitude of DDIs appears relevant. Instead of avoiding drug combinations with DOACs, more DDI trials should be conducted and new strategies such as dose adjustments based on therapeutic drug monitoring should be investigated. However, dose adjustments based on concentration measurements cannot currently be recommended because evidence-based data are missing.

show abstract

Section: Drug-drug Interactions Affecting Doac Therapymentioning

confidence: 99%

Section: Drug-drug Interactions Affecting Doac Therapymentioning

confidence: 99%

Drug–Drug Interactions with Direct Oral Anticoagulants

et al. 2020

View full text Add to dashboard Cite

show abstract

“…Particular care should be taken in the CKD setting where the combination of reduced renal clearance and coadministration of P-glycoprotein inhibitors may increase bleeding risk. 137 Factor Xa DOACs also depend on the Pglycoprotein pathway for metabolism, and interactions with inducers and inhibitors have been described. Moreover, factor Xa DOACs are metabolized by cytochrome P450 and drug effectiveness may be affected by coadministration with CYP3A4 inhibitors (e.g., fluconazole, ketoconazole, itraconazole, and vorconazole) or CYP3A4 inducers (e.g., rifampin and phenytoin).…”

Section: Drug/drug Interactionsmentioning

confidence: 99%

Role of direct oral anticoagulants in patients with kidney disease

Derebail

Rheault

Kerlin

2020

Kidney International

View full text Add to dashboard Cite

The anticoagulation field is experiencing a renaissance that began with regulatory approval of the direct thrombin inhibitor dabigatran, a direct oral anticoagulant (DOAC), in 2010. The DOAC medication class has rapidly evolved to include the additional approval of 4 direct factor Xa inhibitors. Commensurately, DOAC use has increased and collectively account for the majority of new anticoagulant prescriptions. Despite exclusion of patients with moderateto-severe kidney disease from most pivotal DOAC trials, DOACs are increasingly used in this setting. An advantage of DOACs is similar or improved antithrombotic efficacy with less bleeding risk when compared with traditional agents. Several post hoc analyses, retrospective studies, claims data studies, and meta-analyses suggest that these benefits extend to patients with kidney disease. However, the lack of randomized controlled trial data in specific kidney disease settings, with their unique pathophysiology, should be a call to action for the kidney community to systematically study these agents, especially because early data suggest that DOACs may pose less risk of anticoagulant-related nephropathy than do vitamin K antagonists. Most DOACs are renally cleared and are significantly protein bound in circulation; thus, the pharmacokinetics of these drugs are influenced by reduced renal function and proteinuria. DOACs are susceptible to altered metabolism by P-glycoprotein inhibitors and inducers, including drugs commonly used for the management of kidney disease comorbidities. We summarize the currently available literature on DOAC use in kidney disease and illustrate knowledge gaps that represent important opportunities for prospective investigation.

show abstract

“…A few PBPK models for DABE has been published so far. 31,35 Among these, the model developed by Moj et al is comprehensive and can predict DABE, DAB, and DAB-G. However, that model used the salt solubility of DABE (1.8 mg/ml) to develop the absorption model.…”

Section: Discussionmentioning

confidence: 99%

“…A few PBPK models for DABE has been published so far 31,35 . Among these, the model developed by Moj et al is comprehensive and can predict DABE, DAB, and DAB‐G.…”

Section: Discussionmentioning

confidence: 99%