Total and unbound darunavir pharmacokinetics in pregnant women infected with <scp>HIV</scp>‐1: results of a study of darunavir/ritonavir 600/100 mg administered twice daily

Cd, Zorrilla; Wright, Rodney; Osiyemi, OO; Yasin, Salih; Baugh, Bryan; Brown, Kimberley; Coate, Bruce; Verboven, Peter; Mrus, Joseph; Falcon, Ron; Kakuda, Takami

doi:10.1111/hiv.12047

Cited by 47 publications

(50 citation statements)

References 18 publications

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“…There are few published papers about the safety of fosamprenavir [162,163] and darunavir [164] during pregnancy, all reporting infrequent adverse drug reactions in both mothers and infants. These studies all included a small number of volunteers and short follow-up period.…”

Section: Other Antiretroviralsmentioning

confidence: 99%

Adverse drug reactions associated with antiretroviral therapy during pregnancy

Santini-Oliveira

Grinsztejn

2014

Expert Opinion on Drug Safety

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Section: Other Antiretroviralsmentioning

confidence: 99%

Adverse drug reactions associated with antiretroviral therapy during pregnancy

Santini-Oliveira

Grinsztejn

2014

Expert Opinion on Drug Safety

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“…Perhaps, as in the previously cited study of LPV/r, maintenance of the unbound fractions of drug allow for therapeutic antiviral effect. Although total DRV exposure decreased during pregnancy, no clinically relevant change in unbound (active) darunavir occurred, suggesting that no dose adjustment is required for DRV/RTV 600/100 mg bid in pregnant women [43,48].…”

Section: Protease Inhibitors (Pi)mentioning

confidence: 99%

HIV and Pregnancy

Vogler

2014

Curr Treat Options Infect Dis

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“…Clinical data on darunavir use in pregnant women are still limited to small case series, but the available pharmacological data are compatible with our findings. In matched maternal and cord plasma samples at delivery, the median cord/maternal plasma ratios of the darunavir concentrations were, respectively, 0.18 (range, 0.10 to 0.24) (23), 0.11 (24), 0.24 (25), and 0.15 (26).…”

mentioning

confidence: 99%

“…Interestingly, among the protease inhibitors, those which are more lipophilic than darunavir and highly protein bound have lower placental transfer rates (17,31). The protein binding rate for darunavir is 95%, which is considerably less than that for lopinavir or ritonavir and somewhat more than that for atazanavir (26). Darunavir is a substrate of efflux transporters expressed in the placenta, as are the HIV protease inhibitors, in general (32), and some other antiretroviral drugs (18), resulting in decreased fetal exposure (33).…”

mentioning

confidence: 99%

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Placental Transfer of Darunavir in an Ex Vivo Human Cotyledon Perfusion Model

Mandelbrot

Duro

Belissa

et al. 2014

Antimicrob Agents Chemother

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cPlacental transfer of the HIV protease inhibitor darunavir was investigated in 5 term human cotyledons perfused with darunavir (1,000 ng/ml) in the maternal to fetal direction. The mean (؎ the standard deviation [SD]) fetal transfer rate (FTR) (fetal/maternal concentration at steady state from 30 to 90 min) was 15.0% ؎ 2.1%, and the mean (؎SD) clearance index (darunavir FTR/ antipyrine FTR) was 40.3% ؎ 5.8%. This shows that darunavir crosses the placenta at a relatively low rate, resulting in fetal exposure.T he use of antiretroviral drugs has allowed for a spectacular reduction in mother-to-child transmission (MTCT) of HIV in the industrialized countries, with a current rate of Յ0.5% in France (1, 2). Darunavir is an HIV protease inhibitor (PI) that is increasingly used in combination with other drugs to treat HIV infection. It is now considered a first-line option in pregnant women (3, 4), although few data are available to date on its effects during pregnancy. It is classified by the FDA in pregnancy category C (4), meaning that animal studies have failed to demonstrate a risk to the fetus, but there have been no adequate and well-controlled studies in pregnant women. Most of the adverse events described are related to nucleoside reverse transcriptase inhibitors, particularly mitochondrial disease (6) and hematologic or cardiac function toxicities (7), whereas few antiretroviral drugs have shown any relation to the risk of malformations (8). The HIV protease inhibitors are largely well tolerated in utero (9), although there are reports of elevated neonatal bilirubin levels following atazanavir exposure (10) and transient adrenal dysfunction following perinatal lopinavir-ritonavir treatment (11). Determining fetal exposure to a specific drug is important in estimating its potential for preexposure prophylaxis (12), as well as its risk for toxicities in the fetus. Since data from animal studies are difficult to extrapolate to humans due to the differences in placental physiology, human studies are required. There are some data on cord blood concentrations of darunavir at delivery, but these data reflect only a single time point, and larger series are required for population pharmacokinetic modeling (13,14). The ex vivo human cotyledon is an accepted model in which to study and interpret placental transfer (15).The purpose of this study was to investigate the placental transfer of darunavir in the ex vivo human perfused cotyledon.Placentas were collected after uneventful pregnancies and term deliveries (Ն37 weeks gestational age) in a single center (a university hospital maternity department in Colombes, France) and were rapidly perfused on site. Written informed consent was obtained from each woman who donated a placenta, according to French bioethics guidelines (article L1211-2 of the Public Health Code).The darunavir base was provided by the manufacturer (Janssen, Issy-les-Moulineaux, France) as antipyrine-phosphate-buffered saline (PBS). Bradford reagent was purchased from SigmaAldrich (Saint Quentin Fallav...

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Total and unbound darunavir pharmacokinetics in pregnant women infected with HIV‐1: results of a study of darunavir/ritonavir 600/100 mg administered twice daily

Cited by 47 publications

References 18 publications

Adverse drug reactions associated with antiretroviral therapy during pregnancy

Adverse drug reactions associated with antiretroviral therapy during pregnancy

HIV and Pregnancy

Placental Transfer of Darunavir in an Ex Vivo Human Cotyledon Perfusion Model

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