Use of a Bile Salt Export Pump Knockdown Rat Susceptibility Model to Interrogate Mechanism of Drug-Induced Liver Toxicity

Yutai Li; Raymond Evers; Michael J Hafey; Kyeongmi Cheon; Hong Duong; Donna Lynch; Lisa LaFranco-Scheuch; Stephen Pacchione; Alex M Tamburino; Keith Q Tanis; Kristin Geddes; Daniel Holder; Nanyan Rena Zhang; Wen Kang; Raymond J Gonzalez; Alema Galijatovic-Idrizbegovic; Kara M Pearson; Jose A Lebron; Warren E Glaab; Frank D Sistare

doi:10.1093/toxsci/kfz079

Use of a Bile Salt Export Pump Knockdown Rat Susceptibility Model to Interrogate Mechanism of Drug-Induced Liver Toxicity

Toxicol Sci. 2019 Jul 1;170(1):180-198. doi: 10.1093/toxsci/kfz079.

Authors

Yutai Li¹, Raymond Evers², Michael J Hafey², Kyeongmi Cheon³, Hong Duong¹, Donna Lynch¹, Lisa LaFranco-Scheuch¹, Stephen Pacchione¹, Alex M Tamburino⁴, Keith Q Tanis⁴, Kristin Geddes², Daniel Holder³, Nanyan Rena Zhang², Wen Kang¹, Raymond J Gonzalez¹, Alema Galijatovic-Idrizbegovic¹, Kara M Pearson¹, Jose A Lebron¹, Warren E Glaab¹, Frank D Sistare¹

Affiliations

¹ Safety Assessment and Laboratory Animal Resources.
² Pharmacokinetics, Pharmacodynamics and Drug Metabolism.
³ Biometrics Research.
⁴ Genetics and Pharmacogenomics, MRL, West Point, PA 19486.

PMID: 30903168
DOI: 10.1093/toxsci/kfz079

Abstract

Inhibition of the bile salt export pump (BSEP) may be associated with clinical drug-induced liver injury, but is poorly predicted by preclinical animal models. Here we present the development of a novel rat model using siRNA knockdown (KD) of Bsep that displayed differentially enhanced hepatotoxicity to 8 Bsep inhibitors and not to 3 Bsep noninhibitors when administered at maximally tolerated doses for 7 days. Bsep KD alone resulted in 3- and 4.5-fold increases in liver and plasma levels, respectively, of the sum of the 3 most prevalent taurine conjugated bile acids (T3-BA), approximately 90% decrease in plasma and liver glycocholic acid, and a distinct bile acid regulating gene expression pattern, without resulting in hepatotoxicity. Among the Bsep inhibitors, only asunaprevir and TAK-875 resulted in serum transaminase and total bilirubin increases associated with increases in plasma T3-BA that were enhanced by Bsep KD. Benzbromarone, lopinavir, and simeprevir caused smaller increases in plasma T3-BA, but did not result in hepatotoxicity in Bsep KD rats. Bosentan, cyclosporine A, and ritonavir, however, showed no enhancement of T3-BA in plasma in Bsep KD rats, as well as Bsep noninhibitors acetaminophen, MK-0974, or clarithromycin. T3-BA findings were further strengthened through monitoring TCA-d4 converted from cholic acid-d4 overcoming interanimal variability in endogenous bile acids. Bsep KD also altered liver and/or plasma levels of asunaprevir, TAK-875, TAK-875 acyl-glucuronide, benzbromarone, and bosentan. The Bsep KD rat model has revealed differences in the effects on bile acid homeostasis among Bsep inhibitors that can best be monitored using measures of T3-BA and TCA-d4 in plasma. However, the phenotype caused by Bsep inhibition is complex due to the involvement of several compensatory mechanisms.

Keywords: bile acids; bile salt export pump (BSEP); biomarkers; knockdown; liquid chromatography-mass spectrometry (LC-MS); microbiome; transporters.

MeSH terms

ATP Binding Cassette Transporter, Subfamily B, Member 11 / antagonists & inhibitors*
ATP Binding Cassette Transporter, Subfamily B, Member 11 / genetics
Animals
Bilirubin / blood
Chemical and Drug Induced Liver Injury / etiology*
Chemical and Drug Induced Liver Injury / metabolism*
Disease Models, Animal*
Gene Knockdown Techniques
Male
Pharmaceutical Preparations / administration & dosage*
RNA, Small Interfering / genetics
Rats
Rats, Wistar
Taurochenodeoxycholic Acid / blood
Transaminases / blood

Substances

ATP Binding Cassette Transporter, Subfamily B, Member 11
Abcb11 protein, rat
Pharmaceutical Preparations
RNA, Small Interfering
Taurochenodeoxycholic Acid
Transaminases
Bilirubin