Absorption, Metabolism, and Excretion of Darunavir, a New Protease Inhibitor, Administered Alone and with Low-Dose Ritonavir in Healthy Subjects

Vermeir, Marc; Lachau‐Durand, Sophie; Mannens, Geert; Cuyckens, Filip; Hoof, Bart van; Raoof, Araz

doi:10.1124/dmd.108.024109

Cited by 69 publications

(66 citation statements)

References 12 publications

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“…The unbound fraction of drug is considered the only effective fraction available for the diffusion or penetration into tissues. The darunavir plasma free fraction was 7.2% (5.9 to 9.0%) and was consistent with 95% protein binding primarily to plasma alpha 1-acid glycoprotein (21). There was a good correlation between darunavir total and free fractions of plasma proteins (r 2 ϭ 0.827; P Ͻ 0.0001).…”

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confidence: 54%

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Low Frequency of Intermittent HIV-1 Semen Excretion in Patients Treated with Darunavir-Ritonavir at 600/100 Milligrams Twice a Day plus Two Nucleoside Reverse Transcriptase Inhibitors or Monotherapy

Lambert-Niclot

Peytavin

Duvivier

et al. 2010

Antimicrob Agents Chemother

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HIV-1 RNA level and darunavir concentration in the genital tract were measured in 45 men receiving darunavir-ritonavir mono-or tritherapy. At week 48, a low frequency (3/45) of HIV-1 RNA shedding was observed in patients (1 on monotherapy and 2 on triple therapy), although they had undetectable HIV-1 RNA in plasma. The median darunavir seminal plasma concentration was close to the blood plasma free fraction, demonstrating a good penetration of darunavir into the male genital tract.Darunavir-ritonavir is an appropriate candidate for protease inhibitor (PI) monotherapy in maintenance therapy due to its high genetic barrier (5), high potency on naive and resistant HIV strains (11,15), and good pharmacokinetics profile (21). MONOI is an ongoing, 96-week, multicenter, randomized, open-label trial with a primary endpoint at week 48 (W48). This study comprised the first phase, where darunavir at 600/ 100 mg twice daily (b.i.d.) was introduced for 8 weeks as a component of a triple-drug regimen in replacement of the PI, nonnucleoside reverse transcriptase inhibitors (NNRTI), or third nucleoside RTI (NRTI). Patients whose HIV-1 viral load remained lower than 50 copies/ml 4 weeks after darunavir introduction were randomly assigned 1:1 at day 0 (D0) to continue the triple-drug darunavir-containing regimen (darunavir triple therapy) or to stop the two NRTIs (darunavir monotherapy) (12). Available information on antiretroviral drug penetration into the male genital tract is sparse, and concern remains about the efficacy of PI inhibitor monotherapy in viral sanctuaries such as the male genital tract because of the poor penetration of most PIs into semen and the subsequent risk of persistent viral replication and emergence of resistance (4, 7). The aim of our study was to evaluate the outcomes of HIV-1 shedding in the genital tract in patients receiving darunavir-ritonavir monotherapy versus tritherapy and to determine the darunavir concentrations in blood plasma (BP) (free-and total-protein fractions) and seminal plasma (SP) (total-protein fractions).(This work was presented at the 17th Conference on Retroviruses and Opportunistic Infections, San Francisco, CA, 16 to 19 February 2010, poster 610.) From the 225 HIV-1-infected men randomized in the MONOI trial, 47 paired samples of BP and SP were collected at D0 (end of the darunavir tritherapy 8-week run-in period) and W48 after a 3-day period of sexual abstinence. The Cobas TaqMan HIV-1 assay was used to quantify HIV-1 RNA in BP and in SP (at D0 and W48), with limits of quantification of 40 and 200 copies/ml, respectively, as previously described (16,17). Total and free-fraction BP concentrations and total SP darunavir concentrations were determined at D0 and W48 using the ultraperformance liquid chromatography-tandem mass spectrometry (UPLC-MS/MS) method (Acquity UPLC, Acquity TQD) (limit of quantification [LOQ] ϳ 1 ng/ml) as previously described (10). Darunavir plasma protein binding was performed in duplicate using a Centrifree ultrafiltration device. Darunavir concentr...

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confidence: 54%

“…Darunavir-ritonavir is an appropriate candidate for protease inhibitor (PI) monotherapy in maintenance therapy due to its high genetic barrier (5), high potency on naive and resistant HIV strains (11,15), and good pharmacokinetics profile (21). MONOI is an ongoing, 96-week, multicenter, randomized, open-label trial with a primary endpoint at week 48 (W48).…”

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confidence: 99%

Low Frequency of Intermittent HIV-1 Semen Excretion in Patients Treated with Darunavir-Ritonavir at 600/100 Milligrams Twice a Day plus Two Nucleoside Reverse Transcriptase Inhibitors or Monotherapy

Lambert-Niclot

Peytavin

Duvivier

et al. 2010

Antimicrob Agents Chemother

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“…Combined with our data obtained in the present study, these clinical findings support inhibition of presystemic LPV metabolism in human small intestine as a major mechanism underlying the pharmacokinetic boosting of LPV by RTV. In contrast to the 10-fold increase in LPV C max , RTV boosting resulted in a C max increase of only 49 to 77% for IDV (Hill et al, 2009) and 88% for DRV (Vermeir et al, 2009). This increase is lower, than would be expected based on our results obtained in the in situ perfusion experiments, suggesting that data obtained in mice regarding the effect of P-gp inhibition might somewhat overpredict the situation in humans.…”

Section: Discussionmentioning

confidence: 80%

Boosting of HIV Protease Inhibitors by Ritonavir in the Intestine: The Relative Role of Cytochrome P450 and P-Glycoprotein Inhibition Based on Caco-2 Monolayers versus In Situ Intestinal Perfusion in Mice

Holmstock

Annaert²,

Augustijns

2012

Drug Metab Dispos

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ABSTRACT:HIV protease inhibitors are essential components of most recommended treatment regimens for HIV infection. They are always coadministered with ritonavir as a pharmacokinetic booster. Their bioavailability may be impaired because they are substrates of CYP3A4 and several transporters, including P-glycoprotein. The aim of this study was to explore the impact of ritonavir on the intestinal absorption of HIV protease inhibitors in two models: the Caco-2 system and the in situ intestinal perfusion model with mesenteric blood sampling in mice. Using the Caco-2 system, the effect of ritonavir on the permeability of the other HIV protease inhibitors was significant for saquinavir (2-fold increase) and indinavir (3-fold increase), negligible for darunavir and amprenavir, and nonexistent for nelfinavir, lopinavir, tipranavir, and atazanavir.However, performing the in situ intestinal perfusion technique in mice for three selected HIV protease inhibitors showed a significant increase in the intestinal permeability for all: indinavir (3.2-fold), lopinavir (2.3-fold), and darunavir (3-fold). The effect of aminobenzotriazole (a nonspecific cytochrome P450 inhibitor) on lopinavir permeability was comparable with using ritonavir, whereas there was no effect for indinavir and darunavir. We conclude that ritonavir can boost drug absorption by inhibiting P-glycoprotein and/or metabolism, in a compound-specific manner. The results of this study illustrate that a combination of absorption models needs to be considered to elucidate drug-drug interactions at the level of the intestinal mucosa.

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“…Among the HIV PI that have been approved, lopinavir, atazanavir, darunavir and fosamprenavir are most frequently prescribed. 5,6 HIV PI are extensively metabolized by CYP3A enzymes 7,8 and their biliary excretion is mediated by the efflux transporters P-gp (ABCB1) and MRP2 (ABCC2). 8,9 In addition, it has been shown that some HIV PI (or their metabolites) are excreted via the feces for more than 75 %.…”

Section: Introductionmentioning

confidence: 99%

Clearance Prediction of HIV Protease Inhibitors in Man: Role of Hepatic Uptake

Bruyn

Stieger

Augustijns

et al. 2016

Journal of Pharmaceutical Sciences

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The aim of this work was to explore the contribution of the organic anion transporting polypeptide-1B (OATP1B) drug transporters in the hepatic clearance (Cl) of all marketed HIV protease inhibitors (PI) in humans. HIV PI uptake rates in OATP1B1/1B3-transfected Chinese hamster ovary cells were converted to uptake Cl values in human hepatocytes via a relative activity factor, which was determined by comparing uptake of known substrates between OATP1B1/3-transfected cells and human hepatocytes. Metabolic Cl values were determined in human liver microsomes. In vivo hepatic Cl values were calculated either by combining drug uptake and metabolism or based on one of these individual Cl processes and compared with published in vivo hepatic Cl values. Excellent in vitro-in vivo correlation (R(2) = 0.85) was observed when only uptake Cl values were used, but not when only metabolic Cl was used (R(2) = 0.40). The correlation did not improve when both processes were taken into account (R(2) = 0.85). PBPK models confirmed the remarkable sensitivity of predicted exposure to hepatic drug uptake, indicating a key role for OATP1B1/3 in hepatic disposition of several HIV PI in man. This may contribute to the interindividual variability in systemic and hepatic exposure to these drugs in the clinic.

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Absorption, Metabolism, and Excretion of Darunavir, a New Protease Inhibitor, Administered Alone and with Low-Dose Ritonavir in Healthy Subjects

Cited by 69 publications

References 12 publications

Low Frequency of Intermittent HIV-1 Semen Excretion in Patients Treated with Darunavir-Ritonavir at 600/100 Milligrams Twice a Day plus Two Nucleoside Reverse Transcriptase Inhibitors or Monotherapy

Low Frequency of Intermittent HIV-1 Semen Excretion in Patients Treated with Darunavir-Ritonavir at 600/100 Milligrams Twice a Day plus Two Nucleoside Reverse Transcriptase Inhibitors or Monotherapy

Boosting of HIV Protease Inhibitors by Ritonavir in the Intestine: The Relative Role of Cytochrome P450 and P-Glycoprotein Inhibition Based on Caco-2 Monolayers versus In Situ Intestinal Perfusion in Mice

Clearance Prediction of HIV Protease Inhibitors in Man: Role of Hepatic Uptake

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