Abstract
The apparent oral clearance of protease inhibitors (PIs) is increased in pregnant women. Although this phenomenon is reproduced in the mouse, because of the multiplicity of mouse cytochrome P450 isoforms, lack of information on their substrate and inhibitor selectivity, and lack of reagents (e.g., antibodies, purified protein), it is difficult to study the mechanistic basis of this phenomenon in this animal model. To investigate the mechanistic basis of this phenomenon in a more representative model, the nonhuman primate, we first determined whether this phenomenon could be reproduced in Macaca nemestrina, using nelfinavir as a model PI. Consistent with the human and mouse studies, we found that the apparent oral clearance of nelfinavir (NFV) in the macaques was significantly increased (3.14-fold) antepartum (n = 3) versus postpartum (n = 4). This increased apparent oral clearance was a result of an increased systemic clearance (1.9-fold) and a decreased bioavailability (∼45%) during pregnancy. In vitro, pregnancy significantly enhanced the rate of NFV depletion in hepatic, but not intestinal S-9 fractions. Human CYP3A inhibitors erythromycin (0.5 mM), ketoconazole (0.5 μM), and troleandomycin (0.01–1 mM), but not the CYP2C inhibitor, sulfaphenazole (3 μM), significantly inhibited the depletion of NFV in hepatic S-9 fractions and expressed rhesus CYP3A64 enzyme. Based on these data, we conclude that increased hepatic activity of NFV-metabolizing enzymes (perhaps CYP3A enzymes) results in increased clearance of PIs during pregnancy in the macaques. The M. nemestrina should be further investigated as a model to study the mechanisms by which the clearance of PIs is increased during pregnancy.
Footnotes
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This work was supported by the National Institutes of Health National Institute of Child Health & Human Development [Grant P50-HD044404].
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The data presented here have appeared as a Ph.D. thesis: Zhang H (2009) Mechanisms by which pregnancy increases the clearance of the anti-HIV protease inhibitor, nelfinavir. Ph.D. thesis, University of Washington, Seattle, WA.
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This work has been previously presented in part at the following conference: Zhang H, Wu X, Chung F, Naraharisetti SB, Whittington D, Mirfazaelian A, and Unadkat JD (2007) As in humans, pregnancy increases the clearance of the protease inhibitor, nelfinavir, in the nonhuman primate, Macaca nemestrina. 2007 AAPS Annual Meeting and Exposition; 2007 Nov 11–15; San Diego, CA. American Association of Pharmaceutical Scientists, Arlington, VA.
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Article, publication date, and citation information can be found at http://jpet.aspetjournals.org.
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doi:10.1124/jpet.109.151746.
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ABBREVIATIONS: PI, protease inhibitor; NFV, nelfinavir; AUC, area under the curve; P-gp, P-glycoprotein; P450, cytochrome P450; AP, antepartum; PP, postpartum; LC, liquid chromatography; MS, mass spectrometry; ERY, erythromycin; KTZ, ketoconazole; TAO, troleandomycin; SUL, sulfaphenazole; CI, confidence interval.
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↵1 Current affiliation: Department of Biochemistry and Molecular Biology, College of Medicine, University of the Philippines, Manila, Philippines.
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↵2 Current affiliation: Department of Pharmacokinetics, Tehran Chemie Pharmaceutical Co., Tehran, Iran.
- Received February 4, 2009.
- Accepted March 9, 2009.
- The American Society for Pharmacology and Experimental Therapeutics
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