Pharmacokinetic Evaluation of the Interaction between Hepatitis C Virus Protease Inhibitor Boceprevir and 3-Hydroxy-3-Methylglutaryl Coenzyme A Reductase Inhibitors Atorvastatin and Pravastatin

Hulskotte, Ellen; Feng, Hwa‐Ping; Xuan, F.; Gupta, Samir K.; Zutven, M. G. J. A. van; O’Mara, Edward; Wagner, John A.; Butterton, Joan R.

doi:10.1128/aac.02347-12

Cited by 30 publications

(23 citation statements)

References 12 publications

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“…Therefore, the potential of BOC to inhibit atorvastatin gut metabolism might be an additional contributing factor to the increased systemic exposure of atorvastatin. Also consistent with its moderate inhibitory effect on OATP1B1, BOC has been shown to increase the AUC and C max of pravastatin (40 mg) 1.6-and 1.5-fold, respectively (Hulskotte et al, 2011). In humans, pravastatin is eliminated via hepatobiliary and renal excretion mediated by hepatic OATP/MRP2 and renal OAT3, respectively, with minimal metabolism .…”

Section: Discussionmentioning

confidence: 69%

“…This finding suggests that BOC should have lesser impact (versus rifampin) on the hepatic elimination of atorvastatin and other dual substrates of OATP1B/CYP3A where uptake is the rate-determining step. Indeed, a recent clinical DDI study showed that BOC increased plasma atorvastatin AUC and C max 2.3-and 2.7-fold, respectively (Hulskotte et al, 2011). It is noteworthy that atorvastatin has low intestinal availability [Fa*fg (intestinal availability) = 0.24] (Shitara, 2011) in humans, conceivably due to gut CYP3A4 metabolism and Pgp efflux (Hochman et al, 2004).…”

Section: Discussionmentioning

confidence: 99%

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In Vitro Assessment of Drug-Drug Interaction Potential of Boceprevir Associated with Drug Metabolizing Enzymes and Transporters

et al. 2013

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The inhibitory effect of boceprevir (BOC), an inhibitor of hepatitis C virus nonstructural protein 3 protease was evaluated in vitro against a panel of drug-metabolizing enzymes and transporters. BOC, a known substrate for cytochrome P450 (P450) CYP3A and aldoketoreductases, was a reversible time-dependent inhibitor (k inact = 0.12 minute 21, K I = 6.1 mM) of CYP3A4/5 but not an inhibitor of other major P450s, nor of UDP-glucuronosyltransferases 1A1 and 2B7. BOC showed weak to no inhibition of breast cancer resistance protein (BCRP), P-glycoprotein (Pgp), or multidrug resistance protein 2. It was a moderate inhibitor of organic anion transporting polypeptide (OATP) 1B1 and 1B3, with an IC 50 of 18 and 4.9 mM, respectively. In human hepatocytes, BOC inhibited CYP3A-mediated metabolism of midazolam, OATP1B-mediated hepatic uptake of pitavastatin, and both the uptake and metabolism of atorvastatin. The inhibitory potency of BOC was lower than known inhibitors of CYP3A (ketoconazole), OATP1B (rifampin), or both (telaprevir). BOC was a substrate for Pgp and BCRP but not for OATP1B1, OATP1B3, OATP2B1, organic cation transporter, or sodium/taurocholate cotransporting peptide. Overall, our data suggest that BOC has the potential to cause pharmacokinetic interactions via inhibition of CYP3A and CYP3A/OATP1B interplay, with the interaction magnitude lower than those observed with known potent inhibitors. Conversely, pharmacokinetic interactions of BOC, either as a perpetrator or victim, via other major P450s and transporters tested are less likely to be of clinical significance. The results from clinical drug-drug interaction studies conducted thus far are generally supportive of these conclusions.

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Section: Discussionmentioning

confidence: 69%

Section: Discussionmentioning

confidence: 99%

In Vitro Assessment of Drug-Drug Interaction Potential of Boceprevir Associated with Drug Metabolizing Enzymes and Transporters

et al. 2013

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“…Also, Boceprevirmay increase the toxicity of statins via inhibition of OATP1B1 decreasing their hepatic uptake and Simeprevir concentrations may be increased when co-administered with the immunosuppressant cyclosporine due to interaction via transporters. [33,[41][42][43] Because grazoprevir is a substrate of OATP1B1/3, its plasma concentration may be significantly increased by OATP1B1/3 inhibitors (e.g., cyclosporine, lopinavir, saquinavir), and its concurrent use is contraindicated.…”

Section: Pharmacologic Basis Of Direct Acting Antiviral Drug Interactionmentioning

confidence: 99%

Direct acting anti-hepatitis C virus drugs: Clinical pharmacology and future direction

Geddawy

Ibrahim

Elbahie

et al. 2017

Journal of Translational Internal Medicine

138

103

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Chronic hepatitis C virus (HCV) infection is a leading cause of chronic liver disease. The introduction of direct acting antiviral agents (DAAs) for its treatment represents a major advance in terms of sustained virologic response (SVR) rates and adverse effect profiles. Mechanistically, DAAs inhibit specific HCV non-structural proteins (NS) that are vital for its replication. Boceprevir, telaprevir, simeprevir, asunaprevir, grazoprevir and paritaprevir are NS3/4A inhibitors. Ombitasvir, ledipasvir, daclatasvir, elbasvir and velpatasvir are NS5A inhibitors. Sofosbuvir and dasabuvir are NS5B inhibitors. Currently, a combination of two or more DAAs is the corner stone for the treatment of HCV infection. However, the success of DAA therapy is facing several challenges, including the potential of drug-drug interactions and resistant variance. Moreover, the shortage of relevant clinical pharmacological data and drug interaction regarding DAA is a clinical concern. The present review discusses the clinical pharmacology of DAAs with special emphasis on drug-drug interaction.

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“…and C max GMR for the comparison of atorvastatin plus boceprevir vs. atorvastatin alone indicate a 2.3-and 2.7-fold increase, respectively ( Table 2) [45]. Boceprevir exposure was unchanged when coadministered with atorvastatin, with GMRs of 1.04 and 0.96 for boceprevir C max and AUC 8 (Table 3) [45]. The increased C max and AUC of atorvastatin are consistent with increases in atorvastatin exposure seen with other inhibitors of CYP3A4 metabolism, such as erythromycin and itraconazole [46].…”

Section: Atorvastatinmentioning

confidence: 91%

“…The AUC ? and C max GMR for the comparison of atorvastatin plus boceprevir vs. atorvastatin alone indicate a 2.3-and 2.7-fold increase, respectively ( Table 2) [45]. Boceprevir exposure was unchanged when coadministered with atorvastatin, with GMRs of 1.04 and 0.96 for boceprevir C max and AUC 8 (Table 3) [45].…”

Section: Atorvastatinmentioning

confidence: 92%

Clinical Pharmacology Profile of Boceprevir, a Hepatitis C Virus NS3 Protease Inhibitor: Focus on Drug–Drug Interactions

et al. 2015

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Boceprevir is a potent, orally administered ketoamide inhibitor that targets the active site of the hepatitis C virus (HCV) non-structural (NS) 3 protease. The addition of boceprevir to peginterferon plus ribavirin resulted in higher rates of sustained virologic response (SVR) than for peginterferon plus ribavirin alone in phase III studies in both previously treated and untreated patients with HCV infection. Because boceprevir is metabolized by metabolic routes common to many other drugs, and is an inhibitor of cytochrome P450 (CYP) 3A4/5, there is a high potential for drug-drug interactions when boceprevir is administered with other therapies, particularly when treating patients with chronic HCV infection who are often receiving other medications concomitantly. Boceprevir is no longer widely used in the US or EU due to the introduction of second-generation treatments for HCV infection. However, in many other geographic regions, first-generation protease inhibitors such as boceprevir continue to form an important treatment option for patients with HCV infection. This review summarizes the interactions between boceprevir and other therapeutic agents commonly used in this patient population, indicating dose adjustment requirements where needed. Most drug interactions do not affect boceprevir plasma concentrations to a clinically meaningful extent, and thus efficacy is likely to be maintained when boceprevir is coadministered with the majority of other therapeutics. Overall, the drug-drug interaction profile of boceprevir suggests that this agent is suitable for use in a wide range of HCV-infected patients receiving concomitant therapies.

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Pharmacokinetic Evaluation of the Interaction between Hepatitis C Virus Protease Inhibitor Boceprevir and 3-Hydroxy-3-Methylglutaryl Coenzyme A Reductase Inhibitors Atorvastatin and Pravastatin

Cited by 30 publications

References 12 publications

In Vitro Assessment of Drug-Drug Interaction Potential of Boceprevir Associated with Drug Metabolizing Enzymes and Transporters

In Vitro Assessment of Drug-Drug Interaction Potential of Boceprevir Associated with Drug Metabolizing Enzymes and Transporters

Direct acting anti-hepatitis C virus drugs: Clinical pharmacology and future direction

Clinical Pharmacology Profile of Boceprevir, a Hepatitis C Virus NS3 Protease Inhibitor: Focus on Drug–Drug Interactions

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