Evaluation of the Effect of Cobicistat on the<i>In Vitro</i>Renal Transport and Cytotoxicity Potential of Tenofovir

Stray, Kirsten M.; Bam, Rujuta A.; Birkuš, Gabriel; Jia, Hao; Lepist, Eve-Irene; Yant, Stephen R.; Ray, Adrian S.; Cihlář, Tomáš

doi:10.1128/aac.00712-13

Cited by 43 publications

(19 citation statements)

References 29 publications

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“…This recommendation is only made in the case of COBI alone (Tybost Ò ) 'if any coadministered agent (e.g., FTC,3TC,TDF, or adefovir) requires dose adjustment based on creatinine clearance' [46]. All of these are in spite of the fact that the potential for renal drug-drug interactions between COBI and TDF appears to be low, with in vitro and ex vivo data suggesting that the transport mechanisms known to be responsible for the tubular secretion of TDF may be minimally affected by COBI under pharmacologically relevant conditions and tenofovir may have little (if any) effect on MATE-1 or OCT2 [47,48]. DGV, which is considered a second-generation INSTI, may be the most 'complete' drug in its class.…”

Section: Other Aspects Of Instis: Cns Penetration Effects In Reservomentioning

confidence: 99%

HIV integrase inhibitors: a new era in the treatment of HIV

Blanco

Whitlock

Milinkovic

et al. 2015

Expert Opinion on Pharmacotherapy

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Due to their outstanding data of efficacy, tolerability, safety--shared by all three drugs (raltegravir, elvitegravir, dolutegravir) currently belonging to this new family of antiretrovirals--INIs have become part of the recommended initial antiretroviral therapy options. Some differences in dosing, drug-drug interactions and robustness/genetic barrier among the three drugs will provide the physician the characteristics to make the best choice.

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Section: Other Aspects Of Instis: Cns Penetration Effects In Reservomentioning

confidence: 99%

HIV integrase inhibitors: a new era in the treatment of HIV

Blanco

Whitlock

Milinkovic

et al. 2015

Expert Opinion on Pharmacotherapy

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“…Cobicistat increases plasma tenofovir exposure when co-administered with the prodrug tenofovir disoproxil fumarate. This is not considered clinically relevant, and the potential for a pharmacokinetic renal drug-drug interaction is low as both drugs interact primarily with distinct renal transporters, and cobicistat does not interfere with the active renal tubular secretion of tenofovir [42,43]. Cobicistat increased digoxin maximum plasma concentration (C max ) by 41% and exposure (area under the plasma concentrationtime curve [AUC]) by 20% [44].…”

Section: Drug-drug Interactionsmentioning

confidence: 99%

Darunavir/cobicistat once daily for the treatment of HIV

Kakuda

Crauwels

Opsomer

et al. 2015

Expert Review of Anti-infective Therapy

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A current focus in HIV management is improving adherence by minimizing pill burden with convenient formulations, including fixed-dose combinations (FDCs). Darunavir, a HIV protease inhibitor, co-administered with low-dose ritonavir (800/100 mg once daily), is recommended in guidelines in combination with other antiretrovirals for HIV patients with no darunavir resistance-associated mutations. Cobicistat is an alternative agent to ritonavir for boosting plasma drug levels of darunavir among other antiretrovirals. Cobicistat is a more specific cytochrome P450 3A inhibitor than ritonavir without enzyme-inducing properties. This review describes the differing effects of cobicistat and ritonavir on metabolic enzymes, which explains their differing drug-drug interactions, and summarizes some of the studied drug-drug interactions for cobicistat. It also outlines the clinical development and data for a once-daily darunavir/cobicistat FDC. This FDC thus allows for a once-daily treatment regimen (including background antiretrovirals) with reduced pill burden.

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“…For this reason, an increase of 0.05–0.1 mg/dL in plasma creatinine concentrations and a decrease of ~10 mL/min in eGFR CG are expected at week 4 after cobicistat is started. This variation remains stable during treatment with cobicistat and reverts once it is discontinued 21. However, clearance remains unaffected20 when GFR is calculated using standardized methods to assess actual (rather than estimated) clearance, such as iohexol, a substance not secreted or reabsorbed by renal tubule 22.…”

Section: Cobicistat and Kidneysmentioning

confidence: 99%

“…It is worth noting that cobicistat inhibits tubular creatinine secretion, which disturbs renal function estimation without affecting the real glomerular function 21. However, there are several other antiretroviral drugs with a similar effect, such as ritonavir, rilpivirine and dolutegravir, which may also increase plasma creatinine levels due to MATE1 inhibition in the renal tubular cell 36.…”

Section: Use Of Darunavir/cobicistat In the Clinical Practicementioning

confidence: 99%

Profile of once-daily darunavir/cobicistat fixed-dose combination for the treatment of HIV/AIDS

Navarro¹,

Curran²

2016

HIV

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Efficacy is the main objective of antiretroviral treatment and adherence is one of the cornerstones to achieve it. For this reason, treatment simplification is of key importance with regard to antiretroviral regimens. Rezolsta® (darunavir/cobicistat) is the first fixed-dose combination containing a protease inhibitor approved for HIV treatment. This coformulation includes darunavir, a protease inhibitor that has shown its efficacy and safety in naïve and treatment-experienced patients, and cobicistat, the new pharmacokinetic enhancer that is expected to replace ritonavir. Bioequivalence between ritonavir and cobicistat as darunavir boosters has been shown in studies involving healthy volunteers. Furthermore, efficacy and safety of darunavir/cobicistat observed in phase III studies, including naïve and pretreated patients without darunavir-associated resistance mutations, are comparable to historical data of darunavir/ritonavir 800/100 mg once-daily formulation. Adverse events with darunavir/cobicistat are scarce and mild, and basically include skin reactions and gastrointestinal disturbances. Although small increases in plasma creatinine are expected in patients receiving cobicistat due to the inhibition of creatinine transporters in kidney tubules, actual glomerular filtrate rate remains unaltered. Cobicistat does not have an inducer effect on metabolic pathways and shows much more selective inhibition than ritonavir. Therefore, isoenzyms different from CYP3A4 are supposed to be less affected by cobicistat, and thus fewer drug–drug interactions are expected.

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Evaluation of the Effect of Cobicistat on theIn VitroRenal Transport and Cytotoxicity Potential of Tenofovir

Cited by 43 publications

References 29 publications

HIV integrase inhibitors: a new era in the treatment of HIV

HIV integrase inhibitors: a new era in the treatment of HIV

Darunavir/cobicistat once daily for the treatment of HIV

Profile of once-daily darunavir/cobicistat fixed-dose combination for the treatment of HIV/AIDS

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