The Role of PXR Genotype and Transporter Expression in the Placental Transport of Lopinavir in Mice

Lopinavir (LPV), an antiretroviral protease inhibitor frequently prescribed in HIV-positive pregnancies, is a substrate of Abcb1 and Abcc2. As differences in placental expression of these transporters were seen in Pregnane X Receptor (PXR) −/− mice, we examined the impact of placental transporter ex...

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Main Authors: Sarabjit S. Gahir, Micheline Piquette-Miller
Format: Article
Language:English
Published: MDPI AG 2017-10-01
Series:Pharmaceutics
Subjects:
Online Access:https://www.mdpi.com/1999-4923/9/4/49
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spelling doaj-454d0114843947b8b60bcaf458dd435c2020-11-24T21:54:11ZengMDPI AGPharmaceutics1999-49232017-10-01944910.3390/pharmaceutics9040049pharmaceutics9040049The Role of PXR Genotype and Transporter Expression in the Placental Transport of Lopinavir in MiceSarabjit S. Gahir0Micheline Piquette-Miller1Leslie Dan Faculty of Pharmacy, University of Toronto, 144 College Street, Toronto, ON M5S 3M2, CanadaLeslie Dan Faculty of Pharmacy, University of Toronto, 144 College Street, Toronto, ON M5S 3M2, CanadaLopinavir (LPV), an antiretroviral protease inhibitor frequently prescribed in HIV-positive pregnancies, is a substrate of Abcb1 and Abcc2. As differences in placental expression of these transporters were seen in Pregnane X Receptor (PXR) −/− mice, we examined the impact of placental transporter expression and fetal PXR genotype on the fetal accumulation of LPV. PXR +/− dams bearing PXR +/+, PXR +/−, and PXR −/− fetuses were generated by mating PXR +/− female mice with PXR +/− males. On gestational day 17, dams were administered 10 mg/kg LPV (i.v.) and sacrificed 30 min post injection. Concentrations of LPV in maternal plasma and fetal tissue were measured by LC-MS/MS, and transporter expression was determined by quantitative RT-PCR. As compared to the PXR +/+ fetal units, placental expression of Abcb1a, Abcc2, and Abcg2 mRNA were two- to three-fold higher in PXR −/− fetuses (p < 0.05). Two-fold higher fetal:maternal LPV concentration ratios were also seen in the PXR +/+ as compared to the PXR −/− fetuses (p < 0.05), and this significantly correlated to the placental expression of Abcb1a (r = 0.495; p < 0.005). Individual differences in the expression of placental transporters due to genetic or environmental factors can impact fetal exposure to their substrates.https://www.mdpi.com/1999-4923/9/4/49antiretroviralstransportersP-glycoproteinbreast cancer resistance proteinmultidrug resistance associated proteingene regulationprotease inhibitorPregnane X Receptorplacentaknockout mice
collection DOAJ
language English
format Article
sources DOAJ
author Sarabjit S. Gahir
Micheline Piquette-Miller
spellingShingle Sarabjit S. Gahir
Micheline Piquette-Miller
The Role of PXR Genotype and Transporter Expression in the Placental Transport of Lopinavir in Mice
Pharmaceutics
antiretrovirals
transporters
P-glycoprotein
breast cancer resistance protein
multidrug resistance associated protein
gene regulation
protease inhibitor
Pregnane X Receptor
placenta
knockout mice
author_facet Sarabjit S. Gahir
Micheline Piquette-Miller
author_sort Sarabjit S. Gahir
title The Role of PXR Genotype and Transporter Expression in the Placental Transport of Lopinavir in Mice
title_short The Role of PXR Genotype and Transporter Expression in the Placental Transport of Lopinavir in Mice
title_full The Role of PXR Genotype and Transporter Expression in the Placental Transport of Lopinavir in Mice
title_fullStr The Role of PXR Genotype and Transporter Expression in the Placental Transport of Lopinavir in Mice
title_full_unstemmed The Role of PXR Genotype and Transporter Expression in the Placental Transport of Lopinavir in Mice
title_sort role of pxr genotype and transporter expression in the placental transport of lopinavir in mice
publisher MDPI AG
series Pharmaceutics
issn 1999-4923
publishDate 2017-10-01
description Lopinavir (LPV), an antiretroviral protease inhibitor frequently prescribed in HIV-positive pregnancies, is a substrate of Abcb1 and Abcc2. As differences in placental expression of these transporters were seen in Pregnane X Receptor (PXR) −/− mice, we examined the impact of placental transporter expression and fetal PXR genotype on the fetal accumulation of LPV. PXR +/− dams bearing PXR +/+, PXR +/−, and PXR −/− fetuses were generated by mating PXR +/− female mice with PXR +/− males. On gestational day 17, dams were administered 10 mg/kg LPV (i.v.) and sacrificed 30 min post injection. Concentrations of LPV in maternal plasma and fetal tissue were measured by LC-MS/MS, and transporter expression was determined by quantitative RT-PCR. As compared to the PXR +/+ fetal units, placental expression of Abcb1a, Abcc2, and Abcg2 mRNA were two- to three-fold higher in PXR −/− fetuses (p < 0.05). Two-fold higher fetal:maternal LPV concentration ratios were also seen in the PXR +/+ as compared to the PXR −/− fetuses (p < 0.05), and this significantly correlated to the placental expression of Abcb1a (r = 0.495; p < 0.005). Individual differences in the expression of placental transporters due to genetic or environmental factors can impact fetal exposure to their substrates.
topic antiretrovirals
transporters
P-glycoprotein
breast cancer resistance protein
multidrug resistance associated protein
gene regulation
protease inhibitor
Pregnane X Receptor
placenta
knockout mice
url https://www.mdpi.com/1999-4923/9/4/49
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