The influence of co-treatment with carbamazepine, amiodarone and statins on warfarin metabolism and maintenance dose

Herman, Darja; Locatelli, Igor; Grabnar, Iztok; Peternel, Polona; Stegnar, Mojca; Lainščak, Mitja; Mrhar, Aleš; Breskvar, Katja; Dolžan, Vita

doi:10.1007/s00228-006-0104-4

Cited by 43 publications

(38 citation statements)

References 40 publications

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“…129 Several studies have demonstrated reduced warfarin dose requirements, increases in the international normalized ratio (INR), or changes in warfarin metabolite concentrations when coadministered with simvastatin. [130][131][132][133] The magnitude of effect varies, but some reports indicate up to a 30% change in INR, and 1 report showed a doubling of the number of subjects with supratherapeutic INRs. This may be specific to genetic subgroups with low functioning CYP2C9.…”

Section: Anticoagulants Warfarinmentioning

confidence: 99%

See 1 more Smart Citation

Recommendations for Management of Clinically Significant Drug-Drug Interactions With Statins and Select Agents Used in Patients With Cardiovascular Disease: A Scientific Statement From the American Heart Association

Wiggins¹,

Saseen²,

Page³

et al. 2016

Circulation

222

194

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A drug-drug interaction (DDI) is a pharmacokinetic or pharmacological influence of 1 medication on another that differs from the known or anticipated effects of each agent alone.1 A DDI may result in a change in either drug efficacy or drug toxicity for 1 or both of the interacting medications.2 Pharmacokinetic DDIs result in altered absorption, distribution, metabolism, or excretion of a medication. A pharmacodynamic DDI occurs when 1 medication modifies the pharmacological effect of another in an additive, a synergistic, or an antagonistic fashion.It is estimated that ≈2.8% of hospital admissions occur as a direct result of DDIs. 3 However, the actual incidence of hospitalization secondary to clinically significant DDIs is likely to be highly underestimated because medication-related issues are more commonly reported as adverse drug reactions. Complex underlying disease states also may make recognizing a DDI more challenging, further contributing to a lower reported incidence. The overall clinical impact of a DDI can range from mild to life-threatening. Therefore, not all DDIs require a modification in therapy. The variability in the clinical significance of a DDI depends on both medication-specific and patient-specific factors. Medication-specific factors include the individual pharmacokinetic characteristics of each medication implicated in the DDI (eg, binding affinity, half-life [t 1/2 ]), dose of the medications, serum concentrations, timing and sequence of administration, and duration of therapy. Patient-specific factors include age, sex, lifestyle, genetic polymorphisms causing differences in enzyme expression or activity, and disease impairment affecting drug metabolism (eg, hepatic or renal impairment, cardiac failure) or predisposition to differences in efficacy or safety (eg, statin intolerance in patients with a history of myopathy). Clinically significant DDIs are usually preventable. To optimize patient safety, healthcare providers must have an understanding of the mechanisms, magnitude, and potential consequences of any given DDI. Interpreting this information will assist clinicians in the safe prescribing of medications and permits careful consideration of the benefits and risks of concomitant medications.Statins reduce morbidity and mortality in patients with known atherosclerotic cardiovascular disease (ASCVD) and in many primary prevention patients.4-9 Current guidelines recommend high-intensity statin therapy in all patients with ASCVD age ≤75 years and moderate-to high-intensity statin therapy in patients with ASCVD and age >75 years, diabetes mellitus, and familial hypercholesterolemia and in primary prevention patients with 10-year ASCVD risk ≥7.5%.10 Given the important role of statins in patients with ASCVD and those at high ASCVD risk, combination therapy with statins and other cardiovascular medications is highly likely, and potentially significant DDIs must be considered in patients treated with statins.Another important aspect of prescribing medications in combination is evalu...

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Section: Anticoagulants Warfarinmentioning

confidence: 99%

“…140 One study indicated that lovastatin and simvastatin affected warfarin metabolite concentrations. 131 There have been several investigations into a potential rosuvastatinwarfarin interaction. Two studies have shown a significant increase in INR, whereas 1 study did not.…”

Section: Anticoagulants Warfarinmentioning

confidence: 99%

Recommendations for Management of Clinically Significant Drug-Drug Interactions With Statins and Select Agents Used in Patients With Cardiovascular Disease: A Scientific Statement From the American Heart Association

Wiggins¹,

Saseen²,

Page³

et al. 2016

Circulation

222

194

View full text Add to dashboard Cite

show abstract

“…Therefore, the present studies might also help explain some of the drug-drug interactions that have been observed be- Marker protein was prestained with fluorescent dye having an emission maximum at 680 nm (red), whereas the CYP4F2 antibody was conjugated with fluorophore IR800, which emits between 800 and 900 nm (green). tween warfarin and numerous statins (Hickmott et al, 2003;Andrus, 2004;Herman et al, 2006), which provoke an increase in INR and necessitate a decrease in warfarin dose. We speculate that up-regulation of CYP4F2, secondary to statin intake, might be expected to result in an increase in VK1 metabolism, reducing available levels of VK1 and lowering the requirement for warfarin.…”

Section: Cyp4f2 Is a Vitamin K 1 Mono-oxidase 1341mentioning

confidence: 99%

“…Lovastatin decreases accumulated plasma levels of very long-chain fatty acids (Singh et al, 1998), possibly by up-regulating CYP4F2. Of course, although statin-induced inhibition of warfarin metabolism through an interaction with either CYP2C9 or CYP3A4 almost certainly contributes to an increase in patient INR in specific cases (Hickmott et al, 2003), this mechanism alone does not adequately explain the full range of statinwarfarin drug interactions, based on available clinical data (Hickmott et al, 2003;Herman et al, 2006). Finally, based on the current studies, we have modified the pathway view of the vitamin K cycle to include a role for CYP4F2 in "siphoning off" excess vitamin K 1 .…”

Section: Cyp4f2 Is a Vitamin K 1 Mono-oxidase 1341mentioning

confidence: 99%

CYP4F2 Is a Vitamin K₁ Oxidase: An Explanation for Altered Warfarin Dose in Carriers of the V433M Variant

McDonald¹,

Rieder²,

Nakano³

et al. 2009

Mol Pharmacol

281

239

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Genetic polymorphisms in VKORC1 and CYP2C9, genes controlling vitamin K 1 (VK1) epoxide reduction and (S)-warfarin metabolism, respectively, are major contributors to interindividual variability in warfarin dose. The V433M polymorphism (rs2108622) in CYP4F2 has also been associated with warfarin dose and speculatively linked to altered VK1 metabolism. Therefore, the purpose of the present study was to determine the role of CYP4F2 and the V433M polymorphism in the metabolism of VK1 by human liver. In vitro metabolic experiments with accompanying liquid chromatography-tandem mass spectrometry analysis demonstrated that recombinant CYP4F2 (Supersomes) and human liver microsomes supplemented with NADPH converted VK1 to a single product. A screen of all commercially available P450 Supersomes showed that only CYP4F2 was capable of metabolizing VK1 to this product.Steady-state kinetic analysis with recombinant CYP4F2 and with human liver microsomes revealed a substrate K m of 8 to 10 M. Moreover, anti-CYP4F2 IgG, as well as several CYP4F2-selective chemical inhibitors, substantially attenuated the microsomal reaction. Finally, human liver microsomes genotyped for rs2108622 demonstrated reduced vitamin K 1 oxidation and lower CYP4F2 protein concentrations in carriers of the 433M minor allele. These data demonstrate that CYP4F2 is a vitamin K 1 oxidase and that carriers of the CYP4F2 V433M allele have a reduced capacity to metabolize VK1, secondary to an rs2108622-dependent decrease in steady-state hepatic concentrations of the enzyme. Therefore, patients with the rs2108622 polymorphism are likely to have elevated hepatic levels of VK1, necessitating a higher warfarin dose to elicit the same anticoagulant response.

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“…Hence, caution is required when comparing studies using different but apparently selective probes.Third, in addition to drugs with only Level B evidence, the classification of some drugs with Level A evidence requires subjective decisions. For example, the inhibition of CYP2C9 by amiodarone has Level A evidence with an effect at the boundary between moderate and weak inhibition [27][28][29]. Likewise, when only changes in urinary or plasma metabolite ratios are available (as is the case with many older studies for CYP2D6 and CYP2C19 substrates), interactions must be assessed by comparison with other perpetrators for which both metabolite ratios and AUC or clearance data using a recommended probe are reported.…”

Section: Cyp Inhibitorsmentioning

confidence: 99%

Perpetrators of pharmacokinetic drug–drug interactions arising from altered cytochrome P450 activity: a criteria‐based assessment

Polasek

Lin

Miners

et al. 2011

Brit J Clinical Pharma

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WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT• Many drugs inhibit or induce cytochrome P450 enzymes (CYP) to cause clinically significant changes in the concentrations of other drugs, i.e.'perpetrate' pharmacokinetic drug-drug interactions (PK-DDIs).• Tables that list the substrates, inhibitors and inducers of CYP are common, but they lack consistency and are constructed from evidence of variable quality. WHAT THIS STUDY ADDS• This is the first study to catalogue important perpetrators of PK-DDIs using objective criteria and clinical pharmacokinetic drug interaction studies. This information is intended to inform clinical decisions on PK-DDIs.• Existing tables of CYP inhibitors and inducers have low sensitivity and low positive predictive value in identifying the major perpetrators of PK-DDIs. • Several drugs were identified which potentially perpetrate CYP-mediated PK-DDIs, but quality clinical pharmacokinetic interaction studies are lacking. This information may be used to inform future research. AIMSTo catalogue the perpetrators of CYP-mediated pharmacokinetic drug-drug interactions (PK-DDIs) using clinically relevant criteria, and to compare this with an analogous catalogue. METHODSCandidate inhibitors and inducers of CYP1A2, CYP2C9, CYP2C19, CYP2D6 and CYP3A ('perpetrators') were evaluated using published clinical pharmacokinetic interaction studies. Studies were selected on the basis of Նsix human subjects, use of a validated in vivo probe substrate for the CYP enzyme, and clinically relevant dosing. Inhibitors were described according to the FDA classifications of strong, moderate or weak, whereas inducers were classified as major (Նtwofold decrease in AUC) or weak (

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The influence of co-treatment with carbamazepine, amiodarone and statins on warfarin metabolism and maintenance dose

Cited by 43 publications

References 40 publications

Recommendations for Management of Clinically Significant Drug-Drug Interactions With Statins and Select Agents Used in Patients With Cardiovascular Disease: A Scientific Statement From the American Heart Association

Recommendations for Management of Clinically Significant Drug-Drug Interactions With Statins and Select Agents Used in Patients With Cardiovascular Disease: A Scientific Statement From the American Heart Association

CYP4F2 Is a Vitamin K₁ Oxidase: An Explanation for Altered Warfarin Dose in Carriers of the V433M Variant

Perpetrators of pharmacokinetic drug–drug interactions arising from altered cytochrome P450 activity: a criteria‐based assessment

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The influence of co-treatment with carbamazepine, amiodarone and statins on warfarin metabolism and maintenance dose

Cited by 43 publications

References 40 publications

Recommendations for Management of Clinically Significant Drug-Drug Interactions With Statins and Select Agents Used in Patients With Cardiovascular Disease: A Scientific Statement From the American Heart Association

Recommendations for Management of Clinically Significant Drug-Drug Interactions With Statins and Select Agents Used in Patients With Cardiovascular Disease: A Scientific Statement From the American Heart Association

CYP4F2 Is a Vitamin K1 Oxidase: An Explanation for Altered Warfarin Dose in Carriers of the V433M Variant

Perpetrators of pharmacokinetic drug–drug interactions arising from altered cytochrome P450 activity: a criteria‐based assessment

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Product

Resources

About

CYP4F2 Is a Vitamin K₁ Oxidase: An Explanation for Altered Warfarin Dose in Carriers of the V433M Variant