Literature DB >> 30481467

Novel in Vitro Method Reveals Drugs That Inhibit Organic Solute Transporter Alpha/Beta (OSTα/β).

Melina M Malinen1, Antti Kauttonen1,2, James J Beaudoin1, Noora Sjöstedt1, Paavo Honkakoski2, Kim L R Brouwer1.   

Abstract

Drug interactions with the organic solute transporter alpha/beta (OSTα/β) are understudied even though OSTα/β is an important transporter that is expressed in multiple human tissues including the intestine, kidneys, and liver. In this study, an in vitro method to identify novel OSTα/β inhibitors was first developed using OSTα/β-overexpressing Flp-In 293 cells. Incubation conditions were optimized using previously reported OSTα/β inhibitors. A method including a 10 min preincubation step with the test compound was used to screen for OSTα/β inhibition by 77 structurally diverse compounds and fixed-dose combinations. Seven compounds and one fixed-dose combination (100 μM final concentration) inhibited OSTα/β-mediated dehydroepiandrosterone sulfate (DHEAS) uptake by >25%. Concentration-dependent OSTα/β inhibition was evaluated for all putative inhibitors (atorvastatin, ethinylestradiol, fidaxomicin, glycochenodeoxycholate, norgestimate, troglitazone, and troglitazone sulfate). Ethinylestradiol, fidaxomicin, and troglitazone sulfate yielded a clear concentration-inhibition response with IC50 values <200 μM. Among all tested compounds, there was no clear association between physicochemical properties, the severity of hepatotoxicity, and the degree of OSTα/β inhibition. This study utilized a novel in vitro method to identify OSTα/β inhibitors and, for the first time, provided IC50 values for OSTα/β inhibition. These data provide evidence that several drugs, some of which are associated with cholestatic drug-induced liver injury, may impair the function of the OSTα/β transporter.

Entities:  

Keywords:  SLC51A/B; basolateral efflux; bile acid; cholestasis; drug-induced liver injury; inhibition

Mesh:

Substances:

Year:  2018        PMID: 30481467      PMCID: PMC6465078          DOI: 10.1021/acs.molpharmaceut.8b00966

Source DB:  PubMed          Journal:  Mol Pharm        ISSN: 1543-8384            Impact factor:   4.939


  36 in total

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Review 4.  Preincubation-dependent and long-lasting inhibition of organic anion transporting polypeptide (OATP) and its impact on drug-drug interactions.

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Journal:  Pharmacol Ther       Date:  2017-02-27       Impact factor: 12.310

5.  OSTalpha-OSTbeta: a major basolateral bile acid and steroid transporter in human intestinal, renal, and biliary epithelia.

Authors:  Nazzareno Ballatori; Whitney V Christian; Jin Young Lee; Paul A Dawson; Carol J Soroka; James L Boyer; Michael S Madejczyk; Na Li
Journal:  Hepatology       Date:  2005-12       Impact factor: 17.425

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Authors:  Anuradha Rao; Jamie Haywood; Ann L Craddock; Martin G Belinsky; Gary D Kruh; Paul A Dawson
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7.  Organic solute transporter-β (SLC51B) deficiency in two brothers with congenital diarrhea and features of cholestasis.

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8.  Fidaxomicin attains high fecal concentrations with minimal plasma concentrations following oral administration in patients with Clostridium difficile infection.

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Authors:  Courtney B Ferrebee; Jianing Li; Jamie Haywood; Kimberly Pachura; Brian S Robinson; Benjamin H Hinrichs; Rheinallt M Jones; Anuradha Rao; Paul A Dawson
Journal:  Cell Mol Gastroenterol Hepatol       Date:  2018-01-12
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  6 in total

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Review 3.  Novel insights into the organic solute transporter alpha/beta, OSTα/β: From the bench to the bedside.

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4.  Modeling Human Bile Acid Transport and Synthesis in Stem Cell-Derived Hepatocytes with a Patient-Specific Mutation.

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Review 5.  The Role of Uptake and Efflux Transporters in the Disposition of Glucuronide and Sulfate Conjugates.

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6.  Bile Acid Conjugation on Solid Nanoparticles Enhances ASBT-Mediated Endocytosis and Chylomicron Pathway but Weakens the Transcytosis by Inducing Transport Flow in a Cellular Negative Feedback Loop.

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  6 in total

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