Organic Anion Transporter Polypeptide 1B1 Polymorphism Modulates the Extent of Drug–Drug Interaction and Associated Biomarker Levels in Healthy Volunteers

Organic Anion Transporter Polypeptide 1B1 Polymorphism Modulates the Extent of Drug–Drug Interaction and Associated Biomarker Levels in Healthy Volunteers

Understanding transporter‐mediated drug–drug interactions is an integral part of risk assessment in drug development. Recent studies support the use of hexadecanedioate (HDA), tetradecanedioate (TDA), coproporphyrin (CP)‐I, and CP‐III as clinical biomarkers for evaluating organic anion‐transporting...

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Main Authors: Sook Wah Yee, Marilyn M. Giacomini, Hong Shen, W. Griffith Humphreys, Howard Horng, William Brian, Yurong Lai, Deanna L. Kroetz, Kathleen M. Giacomini
Format: Article
Language:English
Published: Wiley 2019-07-01
Series:Clinical and Translational Science
Online Access:https://doi.org/10.1111/cts.12625
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spelling doaj-7aec9e736d274c7e909b1eb4fcb6398c2020-11-25T00:24:50ZengWileyClinical and Translational Science1752-80541752-80622019-07-0112438839910.1111/cts.12625Organic Anion Transporter Polypeptide 1B1 Polymorphism Modulates the Extent of Drug–Drug Interaction and Associated Biomarker Levels in Healthy VolunteersSook Wah Yee0Marilyn M. Giacomini1Hong Shen2W. Griffith Humphreys3Howard Horng4William Brian5Yurong Lai6Deanna L. Kroetz7Kathleen M. Giacomini8Department of Bioengineering and Therapeutic Sciences University of California San Francisco California USADrug Metabolism Department Gilead Sciences, Inc. Foster City California USADepartment of Metabolism and Pharmacokinetics Bristol‐Myers Squibb Research and Development Princeton New Jersey USADepartment of Metabolism and Pharmacokinetics Bristol‐Myers Squibb Research and Development Princeton New Jersey USADepartment of Bioengineering and Therapeutic Sciences University of California San Francisco California USADisposition Safety and Animal Research Sanofi‐Aventis Great Valley Pennsylvania USADrug Metabolism Department Gilead Sciences, Inc. Foster City California USADepartment of Bioengineering and Therapeutic Sciences University of California San Francisco California USADepartment of Bioengineering and Therapeutic Sciences University of California San Francisco California USAUnderstanding transporter‐mediated drug–drug interactions is an integral part of risk assessment in drug development. Recent studies support the use of hexadecanedioate (HDA), tetradecanedioate (TDA), coproporphyrin (CP)‐I, and CP‐III as clinical biomarkers for evaluating organic anion‐transporting polypeptide (OATP)1B1 (SLCO1B1) inhibition. The current study investigated the effect of OATP1B1 genotype c.521T>C (OATP1B1‐Val174Ala) on the extent of interaction between cyclosporin A (CsA) and pravastatin, and associated endogenous biomarkers of the transporter (HDA, TDA, CP‐I, and CP‐III), in 20 healthy volunteers. The results show that the levels of each clinical biomarker and pravastatin were significantly increased in plasma samples of the volunteers following administration of pravastatin plus CsA compared with pravastatin plus placebo. The overall fold change in the area under the concentration–time curve (AUC) and maximum plasma concentration (Cmax) was similar among the four biomarkers (1.8–2.5‐fold, paired t‐test P value < 0.05) in individuals who were homozygotes or heterozygotes of the major allele, c.521T. However, the fold change in AUC and Cmax for HDA and TDA was significantly abolished in the subjects who were c.521‐CC, whereas the respective fold change in AUC and Cmax for pravastatin and CP‐I and CP‐III were slightly weaker in individuals who were c.521‐CC compared with c.521‐TT/TC genotypes. In addition, this study provides the first evidence that SLCO1B1 c.521T>C genotype is significantly associated with CP‐I but not CP‐III levels. Overall, these results suggest that OATP1B1 genotype can modulate the effects of CsA on biomarker levels; the extent of modulation differs among the biomarkers.https://doi.org/10.1111/cts.12625
collection DOAJ
language English
format Article
sources DOAJ
author Sook Wah Yee
Marilyn M. Giacomini
Hong Shen
W. Griffith Humphreys
Howard Horng
William Brian
Yurong Lai
Deanna L. Kroetz
Kathleen M. Giacomini
spellingShingle Sook Wah Yee
Marilyn M. Giacomini
Hong Shen
W. Griffith Humphreys
Howard Horng
William Brian
Yurong Lai
Deanna L. Kroetz
Kathleen M. Giacomini
Organic Anion Transporter Polypeptide 1B1 Polymorphism Modulates the Extent of Drug–Drug Interaction and Associated Biomarker Levels in Healthy Volunteers
Clinical and Translational Science
author_facet Sook Wah Yee
Marilyn M. Giacomini
Hong Shen
W. Griffith Humphreys
Howard Horng
William Brian
Yurong Lai
Deanna L. Kroetz
Kathleen M. Giacomini
author_sort Sook Wah Yee
title Organic Anion Transporter Polypeptide 1B1 Polymorphism Modulates the Extent of Drug–Drug Interaction and Associated Biomarker Levels in Healthy Volunteers
title_short Organic Anion Transporter Polypeptide 1B1 Polymorphism Modulates the Extent of Drug–Drug Interaction and Associated Biomarker Levels in Healthy Volunteers
title_full Organic Anion Transporter Polypeptide 1B1 Polymorphism Modulates the Extent of Drug–Drug Interaction and Associated Biomarker Levels in Healthy Volunteers
title_fullStr Organic Anion Transporter Polypeptide 1B1 Polymorphism Modulates the Extent of Drug–Drug Interaction and Associated Biomarker Levels in Healthy Volunteers
title_full_unstemmed Organic Anion Transporter Polypeptide 1B1 Polymorphism Modulates the Extent of Drug–Drug Interaction and Associated Biomarker Levels in Healthy Volunteers
title_sort organic anion transporter polypeptide 1b1 polymorphism modulates the extent of drug–drug interaction and associated biomarker levels in healthy volunteers
publisher Wiley
series Clinical and Translational Science
issn 1752-8054
1752-8062
publishDate 2019-07-01
description Understanding transporter‐mediated drug–drug interactions is an integral part of risk assessment in drug development. Recent studies support the use of hexadecanedioate (HDA), tetradecanedioate (TDA), coproporphyrin (CP)‐I, and CP‐III as clinical biomarkers for evaluating organic anion‐transporting polypeptide (OATP)1B1 (SLCO1B1) inhibition. The current study investigated the effect of OATP1B1 genotype c.521T>C (OATP1B1‐Val174Ala) on the extent of interaction between cyclosporin A (CsA) and pravastatin, and associated endogenous biomarkers of the transporter (HDA, TDA, CP‐I, and CP‐III), in 20 healthy volunteers. The results show that the levels of each clinical biomarker and pravastatin were significantly increased in plasma samples of the volunteers following administration of pravastatin plus CsA compared with pravastatin plus placebo. The overall fold change in the area under the concentration–time curve (AUC) and maximum plasma concentration (Cmax) was similar among the four biomarkers (1.8–2.5‐fold, paired t‐test P value < 0.05) in individuals who were homozygotes or heterozygotes of the major allele, c.521T. However, the fold change in AUC and Cmax for HDA and TDA was significantly abolished in the subjects who were c.521‐CC, whereas the respective fold change in AUC and Cmax for pravastatin and CP‐I and CP‐III were slightly weaker in individuals who were c.521‐CC compared with c.521‐TT/TC genotypes. In addition, this study provides the first evidence that SLCO1B1 c.521T>C genotype is significantly associated with CP‐I but not CP‐III levels. Overall, these results suggest that OATP1B1 genotype can modulate the effects of CsA on biomarker levels; the extent of modulation differs among the biomarkers.
url https://doi.org/10.1111/cts.12625
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