Current insights in the complexities underlying drug-induced cholestasis

Deferm, Neel; Vocht, Tom De; Qi, Bing; Brantegem, Pieter Van; Gijbels, Eva; Vinken, Mathieu; Witte, Peter de; Bouillon, Thomas; Annaert, Pieter

doi:10.1080/10408444.2019.1635081

Cited by 21 publications

(19 citation statements)

References 228 publications

(251 reference statements)

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“…Preclinical assays for DIC detection often rely on evaluation of the test compound towards individual cellular targets such as their inhibitory potential towards the bile salt export pump (BSEP) by using BSEP membrane vesicles [2 , 3] . However, the underlying mechanisms of DIC development are more complex involving multiple other transporters and nuclear receptors [4] . A more comprehensive in vitro model such as sandwich-cultured human hepatocytes (SCHH) are more suited due to the presence of metabolizing enzymes and transporters relevant to bile salt disposition [5] .…”

Section: General Description Of the Methodsmentioning

confidence: 99%

Drug-induced cholestasis assay in primary hepatocytes

Brantegem

Chatterjee

Bruyn³

et al. 2020

MethodsX

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Drug-induced cholestasis (DIC) is a major cause of clinical failure of drug candidates. Numerous patients worldwide are affected when exposed to marketed drugs exhibiting a DIC signature. Prospective identification of DIC during early compound development remains challenging. Here we describe the optimized in vitro procedure for early assessment and prediction of an increased DIC risk. Our method is based on three principles: Exposure of primary human hepatocyte cultures to test compounds in the absence and presence of a physiologically relevant mixture of endogenous bile salts. Rapid and quantitative assessment of the influence of concomitant bile salt exposure on hepatocyte functionality and integrity after 24 h or 48 h of incubation. Translation of the in vitro result, expressed as a DIC index (DICI) value, into an in vivo safety margin. Using our historical control data, a new (data driven) DICI cut-off value of 0.78 was established for discerning cholestatic and non-cholestatic compounds. Our DIC assay protocol was further improved by now relying on the principle of the no observable adverse effect level (NOAEL) for determining the highest test compound concentration corresponding to a DICI ≥ 0.78. Predicted safety margin values were subsequently calculated for compounds displaying hepatotoxic and/or cholestatic effects in patients, thus enabling evaluation of the performance of our DIC assay. Of note, this assay can be extended to explore the role of drug metabolites in precipitating DIC.

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Section: General Description Of the Methodsmentioning

confidence: 99%

Drug-induced cholestasis assay in primary hepatocytes

Brantegem

Chatterjee

Bruyn³

et al. 2020

MethodsX

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“…We also studied selected systematic reviews and guidelines describing types of DILI 13,14,32 as well as articles explaining potential drug-drug interactions associated with membrane transporters. 15,16,[33][34][35][36][37] Anastrozole is a substrate for the CYP3A4 enzyme, but it is not a substrate for the P-glycoprotein. Amlodipine and gliquidone were identified as inhibitors of both the CYP3A4 enzyme and P-glycoprotein, which could result in an increase in systemic exposure to drugs that are substrates for CYP3A4 and P-glycoprotein.…”

Section: Pharmacological Point Of Viewmentioning

confidence: 99%

“…Wishart et al, 4 Konig et al, 33 Deferm et al, 37 Jansen, 54 Fernández-Murga et al 55 Hepatocyte membrane 4 Yang et al 16 Giacomini and Sugiyama, 40 Hu et al, 41 Corsini and Keppler, 35 Deferm et al, 37 Kock et al, 47 Ivanyuk et al 53 4 Weiss et al, 36 Hu et al, 41 Ivanyuk et al 53 The other drugs were taken before admission to the hospital and also in the hospital. BCRP/ABCG2, breast cancer resistant protein/ATP-binding cassette subfamily G2; BSEP/ABCB-11, bile salt export pump/ATP-binding cassette protein subfamily B-11; MDR-1, multidrug resistance protein-1 or P-glycoprotein is an expression for ABCB1; MRP-2/ABCC2, multidrug resistance-associated protein-2/ATP-binding cassette protein subfamily C 2; MRP-3/ABCC3, multidrug resistance-associated protein-3/ATP-binding cassette protein subfamily C-3; MRP-4/ABCC4, multidrug resistance-associated protein-4/ATP-binding cassette protein subfamily C-4; NTCP, sodium taurocholate co-transporter polypeptide that is, solute carrier family 10 transporter A1; OATP1B1, organic anion transport protein 1B1 that is, SLCO 1B1, solute carrier organic anion transporter family member 1B1; OCT1, organic cation transporter, that is, SLC22A1, solute carrier family 22 transporter A1; OCTN2, organic cation/carnitine transporter.…”

Section: Abc B11mentioning

confidence: 99%

Drug-induced liver injury after switching from tamoxifen to anastrozole in a patient with a history of breast cancer being treated for hypertension and diabetes

Potměšil

Szotkowská

2020

Therapeutic Advances in Chronic Disease

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Anastrozole is a selective non-steroidal aromatase inhibitor that blocks the conversion of androgens to estrogens in peripheral tissues. It is used as adjuvant therapy for early-stage hormone-sensitive breast cancer in postmenopausal women. Significant side effects of anastrozole include osteoporosis and increased levels of cholesterol. To date, seven case reports on anastrozole hepatotoxicity have been published. We report the case of an 81-year-old woman with a history of breast cancer, arterial hypertension, type 2 diabetes mellitus, hyperlipidemia, and chronic renal insufficiency. Four days after switching hormone therapy from tamoxifen to anastrozole, icterus developed along with a significant increase in liver enzymes (measured in the blood). The patient was admitted to hospital, where a differential diagnosis of jaundice was made and anastrozole was withdrawn. Subsequently, hepatic functions quickly normalized. The observed liver injury was attributed to anastrozole since other possible causes of jaundice were excluded. However, concomitant pharmacotherapy could have contributed to the development of jaundice and hepatotoxicity, after switching from tamoxifen to anastrozole since several the patient’s medications were capable of inhibiting hepatobiliary transport of bilirubin, bile acids, and metabolized drugs through inhibition of ATP-binding cassette proteins. Telmisartan, tamoxifen, and metformin all block bile salt efflux pumps. The efflux function of multidrug resistance protein 2 is known to be reduced by telmisartan and tamoxifen and breast cancer resistance protein is known to be inhibited by telmisartan and amlodipine. Moreover, the activity of P-glycoprotein transporters are known to be decreased by telmisartan, amlodipine, gliquidone, as well as the previously administered tamoxifen. Finally, the role of genetic polymorphisms of cytochrome P450 enzymes and/or drug transporters cannot be ruled out since the patient was not tested for polymorphisms.

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“…Importantly, our analysis in MPCCs does not consider the type of DILI associated with a compound, but rather focuses on potential to inhibit biliary efflux. Since inhibition of biliary efflux is only one potential mechanism causing/correlating with cholestatic liver injury (Balistreri et al, 2005, Burbank et al, 2016, Deferm et al, 2019, compounds known to be cholestatic in humans such as troglitazone, nefazodone, and bosentan may or may not be flagged using a 10-fold cutoff between the TCA BEI IC 50 and fu*I in,max indicating altered transporter-mediated efflux.…”

Section: Discussionmentioning

confidence: 99%

A Two-Tiered In Vitro Approach to De-Risk Drug Candidates for Potential Bile Salt Export Pump Inhibition Liabilities in Drug Discovery

et al. 2020

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Hepatocellular accumulation of bile salts by inhibition of bile salt export pump (BSEP/ABCB11) may result in cholestasis and is one proposed mechanism of drug induced liver injury (DILI). To understand the relationship between BSEP inhibition and DILI, we evaluated 64 DILI positive and 57 DILI negative compounds in BSEP, multidrug resistance protein 2 (MRP2), MRP3, and MRP4 vesicular inhibition assays. An empirical cutoff (5 μM) for BSEP inhibition was established based on a relationship between BSEP IC 50 values and the calculated maximal unbound concentration at the inlet of the human liver (fu*I in,max , assay specificity = 98%). Including inhibition of MRP2-4 did not increase DILI predictivity. To further understand the potential to inhibit bile salt transport, a selected subset of 30 compounds were tested for inhibition of taurocholate (TCA) transport in a long-term human hepatocyte micropatterned coculture (MPCC) system. The resulting IC 50 for TCA in vitro biliary clearance (Cl biliary) and biliary excretion index (BEI) in MPCCs were compared to the compound's fu*I in,max to assess potential risk for bile salt transport perturbation. The data show high specificity (89%). Nine out of 15 compounds showed an IC 50 value in the BSEP vesicular assay of <5μM, but the BEI IC 50 was greater than 10-fold the fu*I in,max , suggesting that inhibition of BSEP in vivo is unlikely. The data indicate that although BSEP inhibition measured in membrane vesicles correlates with DILI risk, that measurement of this assay activity is insufficient. A two-tiered strategy incorporating MPCCs is presented to reduce BSEP inhibition potential and improve DILI risk. Statement of Significance This work describes a two-tiered in vitro approach to de-risk compounds for potential bile salt export pump inhibition liabilities in drug discovery utilizing membrane vesicles and a long-term human hepatocyte micropatterned co-culture system. Cutoffs to maximize specificity were established based on in vitro data from a set of 121 DILI positive and negative compounds and associated calculated maximal unbound concentration at the inlet of the human liver (fu*I in,max) based on the highest clinical dose.

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Current insights in the complexities underlying drug-induced cholestasis

Cited by 21 publications

References 228 publications

Drug-induced cholestasis assay in primary hepatocytes

Drug-induced cholestasis assay in primary hepatocytes

Drug-induced liver injury after switching from tamoxifen to anastrozole in a patient with a history of breast cancer being treated for hypertension and diabetes

A Two-Tiered In Vitro Approach to De-Risk Drug Candidates for Potential Bile Salt Export Pump Inhibition Liabilities in Drug Discovery

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