Evaluating Hepatobiliary Transport with (18)F-Labeled Bile Acids: The Effect of Radiolabel Position and Bile Acid Structure on Radiosynthesis and In Vitro and In Vivo Performance

INTRODUCTION: An in vivo determination of bile acid hepatobiliary transport efficiency can be of use in liver disease and preclinical drug development. Given the increased interest in bile acid Positron Emission Tomography- (PET-) imaging, a further understanding of the impact of 18-fluorine substit...

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Autores principales: De Lombaerde, Stef, Kersemans, Ken, Neyt, Sara, Verhoeven, Jeroen, Vanhove, Christian, De Vos, Filip
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5941726/
https://www.ncbi.nlm.nih.gov/pubmed/29853807
http://dx.doi.org/10.1155/2018/6345412
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author De Lombaerde, Stef
Kersemans, Ken
Neyt, Sara
Verhoeven, Jeroen
Vanhove, Christian
De Vos, Filip
author_facet De Lombaerde, Stef
Kersemans, Ken
Neyt, Sara
Verhoeven, Jeroen
Vanhove, Christian
De Vos, Filip
author_sort De Lombaerde, Stef
collection PubMed
description INTRODUCTION: An in vivo determination of bile acid hepatobiliary transport efficiency can be of use in liver disease and preclinical drug development. Given the increased interest in bile acid Positron Emission Tomography- (PET-) imaging, a further understanding of the impact of 18-fluorine substitution on bile acid handling in vitro and in vivo can be of significance. METHODS: A number of bile acid analogues were conceived for nucleophilic substitution with [(18)F]fluoride: cholic acid analogues of which the 3-, 7-, or 12-OH function is substituted with a fluorine atom (3α-[(18)F]FCA; 7β-[(18)F]FCA; 12β-[(18)F]FCA); a glycocholic and chenodeoxycholic acid analogue, substituted on the 3-position (3β-[(18)F]FGCA and 3β-[(18)F]FCDCA, resp.). Uptake by the bile acid transporters NTCP and OATP1B1 was evaluated with competition assays in transfected CHO and HEK cell lines and efflux by BSEP in membrane vesicles. PET-scans with the tracers were performed in wild-type mice (n = 3 per group): hepatobiliary transport was monitored and compared to a reference tracer, namely, 3β-[(18)F]FCA. RESULTS: Compounds 3α-[(18)F]FCA, 3β-[(18)F]FGCA, and 3β-[(18)F]FCDCA were synthesized in moderate radiochemical yields (4–10% n.d.c.) and high radiochemical purity (>99%); 7β-[(18)F]FCA and 12β-[(18)F]FCA could not be synthesized and included further in this study. In vitro evaluation showed that 3α-FCA, 3β-FGCA, and 3β-FCDCA all had a low micromolar Ki-value for NTCP, OATP1B1, and BSEP. In vivo, 3α-[(18)F]FCA, 3β-[(18)F]FGCA, and 3β-[(18)F]FCDCA displayed hepatobiliary transport with varying efficiency. A slight yet significant difference in uptake and efflux rate was noticed between the 3α-[(18)F]FCA and 3β-[(18)F]FCA epimers. Conjugation of 3β-[(18)F]FCA with glycine had no significant effect in vivo. Compound 3β-[(18)F]FCDCA showed a significantly slower hepatic uptake and efflux towards gallbladder and intestines. CONCLUSION: A set of (18)F labeled bile acids was synthesized that are substrates of the bile acid transporters in vitro and in vivo and can serve as PET-biomarkers for hepatobiliary transport of bile acids.
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spelling pubmed-59417262018-05-31 Evaluating Hepatobiliary Transport with (18)F-Labeled Bile Acids: The Effect of Radiolabel Position and Bile Acid Structure on Radiosynthesis and In Vitro and In Vivo Performance De Lombaerde, Stef Kersemans, Ken Neyt, Sara Verhoeven, Jeroen Vanhove, Christian De Vos, Filip Contrast Media Mol Imaging Research Article INTRODUCTION: An in vivo determination of bile acid hepatobiliary transport efficiency can be of use in liver disease and preclinical drug development. Given the increased interest in bile acid Positron Emission Tomography- (PET-) imaging, a further understanding of the impact of 18-fluorine substitution on bile acid handling in vitro and in vivo can be of significance. METHODS: A number of bile acid analogues were conceived for nucleophilic substitution with [(18)F]fluoride: cholic acid analogues of which the 3-, 7-, or 12-OH function is substituted with a fluorine atom (3α-[(18)F]FCA; 7β-[(18)F]FCA; 12β-[(18)F]FCA); a glycocholic and chenodeoxycholic acid analogue, substituted on the 3-position (3β-[(18)F]FGCA and 3β-[(18)F]FCDCA, resp.). Uptake by the bile acid transporters NTCP and OATP1B1 was evaluated with competition assays in transfected CHO and HEK cell lines and efflux by BSEP in membrane vesicles. PET-scans with the tracers were performed in wild-type mice (n = 3 per group): hepatobiliary transport was monitored and compared to a reference tracer, namely, 3β-[(18)F]FCA. RESULTS: Compounds 3α-[(18)F]FCA, 3β-[(18)F]FGCA, and 3β-[(18)F]FCDCA were synthesized in moderate radiochemical yields (4–10% n.d.c.) and high radiochemical purity (>99%); 7β-[(18)F]FCA and 12β-[(18)F]FCA could not be synthesized and included further in this study. In vitro evaluation showed that 3α-FCA, 3β-FGCA, and 3β-FCDCA all had a low micromolar Ki-value for NTCP, OATP1B1, and BSEP. In vivo, 3α-[(18)F]FCA, 3β-[(18)F]FGCA, and 3β-[(18)F]FCDCA displayed hepatobiliary transport with varying efficiency. A slight yet significant difference in uptake and efflux rate was noticed between the 3α-[(18)F]FCA and 3β-[(18)F]FCA epimers. Conjugation of 3β-[(18)F]FCA with glycine had no significant effect in vivo. Compound 3β-[(18)F]FCDCA showed a significantly slower hepatic uptake and efflux towards gallbladder and intestines. CONCLUSION: A set of (18)F labeled bile acids was synthesized that are substrates of the bile acid transporters in vitro and in vivo and can serve as PET-biomarkers for hepatobiliary transport of bile acids. Hindawi 2018-04-23 /pmc/articles/PMC5941726/ /pubmed/29853807 http://dx.doi.org/10.1155/2018/6345412 Text en Copyright © 2018 Stef De Lombaerde et al. https://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
De Lombaerde, Stef
Kersemans, Ken
Neyt, Sara
Verhoeven, Jeroen
Vanhove, Christian
De Vos, Filip
Evaluating Hepatobiliary Transport with (18)F-Labeled Bile Acids: The Effect of Radiolabel Position and Bile Acid Structure on Radiosynthesis and In Vitro and In Vivo Performance
title Evaluating Hepatobiliary Transport with (18)F-Labeled Bile Acids: The Effect of Radiolabel Position and Bile Acid Structure on Radiosynthesis and In Vitro and In Vivo Performance
title_full Evaluating Hepatobiliary Transport with (18)F-Labeled Bile Acids: The Effect of Radiolabel Position and Bile Acid Structure on Radiosynthesis and In Vitro and In Vivo Performance
title_fullStr Evaluating Hepatobiliary Transport with (18)F-Labeled Bile Acids: The Effect of Radiolabel Position and Bile Acid Structure on Radiosynthesis and In Vitro and In Vivo Performance
title_full_unstemmed Evaluating Hepatobiliary Transport with (18)F-Labeled Bile Acids: The Effect of Radiolabel Position and Bile Acid Structure on Radiosynthesis and In Vitro and In Vivo Performance
title_short Evaluating Hepatobiliary Transport with (18)F-Labeled Bile Acids: The Effect of Radiolabel Position and Bile Acid Structure on Radiosynthesis and In Vitro and In Vivo Performance
title_sort evaluating hepatobiliary transport with (18)f-labeled bile acids: the effect of radiolabel position and bile acid structure on radiosynthesis and in vitro and in vivo performance
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5941726/
https://www.ncbi.nlm.nih.gov/pubmed/29853807
http://dx.doi.org/10.1155/2018/6345412
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