Current Challenges and Controversies in Drug-Induced Liver Injury

Corsini, Alberto; Ganey, Patricia E.; Ju, Cynthia; Kaplowitz, Neil; Pessayre, Dominique; Roth, Robert A.; Watkins, Paul B.; Albassam, Mudher; Liu, Baolian; Stancic, Saray; Suter, Laura; Bortolini, M.

doi:10.1007/bf03261997

Cited by 54 publications

(32 citation statements)

References 136 publications

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“…This is particularly true for hepatotoxicity, which is a leading cause of compound failure during the preclinical and clinical stages of development. [4][5][6] High-content imaging has been demonstrated to be particular useful for hepatotoxicity testing as it can assess subtle phenotypic changes and provide multiparametric read outs. 25,26 In the present work,…”

Section: Discussionmentioning

confidence: 99%

“…In fact, drug-induced liver injury has been associated with over a third of acute liver failures in the United States and more than 1,000 drugs are considered potentially toxic to the liver. 2,3 Drug-induced liver injury is one of the major causes of drug candidate failure in preclinical and clinical testing 4 and is also the most frequently cited reason for withdrawal of approved drugs. 5,6 While in vivo animal studies remain the standard for toxicity testing, they are time consuming and costly, and more importantly, are rather poor predictors of human toxicity.…”

Section: Introductionmentioning

confidence: 99%

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High-Content Assays for Hepatotoxicity Using Induced Pluripotent Stem Cell–Derived Cells

Sirenko¹,

Hesley²,

Rusyn

et al. 2014

ASSAY and Drug Development Technologies

117

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Development of predictive in vitro assays for early toxicity evaluation is extremely important for improving the drug development process and reducing drug attrition rates during clinical development. High-content imaging-based in vitro toxicity assays are emerging as efficient tools for safety and efficacy testing to improve drug development efficiency. In this report we have used an induced pluripotent stem cell (iPSC)-derived hepatocyte cell model having a primary tissue-like phenotype, unlimited availability, and the potential to compare cells from different individuals. We examined a number of assays and phenotypic markers and developed automated screening methods for assessing multiparameter readouts of general and mechanism-specific hepatotoxicity. Endpoints assessed were cell viability, nuclear shape, average and integrated cell area, mitochondrial membrane potential, phospholipid accumulation, cytoskeleton integrity, and apoptosis. We assayed compounds with known mechanisms of toxicity and also evaluated a diverse hepatotoxicity library of 240 compounds. We conclude that high-content automated screening assays using iPSC-derived hepatocytes are feasible, provide information about mechanisms of toxicity, and can facilitate the safety assessment of drugs and chemicals.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

High-Content Assays for Hepatotoxicity Using Induced Pluripotent Stem Cell–Derived Cells

Sirenko¹,

Hesley²,

Rusyn

et al. 2014

ASSAY and Drug Development Technologies

117

View full text Add to dashboard Cite

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“…We used GGT and ALP as additional biomarkers to evaluate each patient's liver function. 17 Secondary outcome measures included the occurrence of adverse drug reactions, prolonged treatment duration, taking second-line drugs, and the clearance of tuberculosis bacteria from the sputum after 2 months of treatment.…”

Section: Methodsmentioning

confidence: 99%

Preventive use of a hepatoprotectant against anti‐tuberculosis drug‐induced liver injury: A randomized controlled trial

Zhang

Pan²,

Peng

et al. 2016

J of Gastro and Hepatol

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Background and Aim: Hepatoprotectants are routinely prescribed in China to prevent anti-tuberculosis drug-induced liver injury (ATLI). However, their biological mechanismshave not yet been clearly demonstrated. This study aims to evaluate the preventive effects of Silybum marianum against drug-induced liver injury among tuberculosis patients and to provide clinical guidelines for tuberculosis management in China. Methods: A randomized controlled trial was performed in Jiangsu, China. Tuberculosis patients were randomly allocated to the experimental group (anti-tuberculosis therapy plus S. marianum capsule) or the control group (anti-tuberculosis therapy plus vitamin C tablet). The primary outcomes were the occurrence of probable and possible ATLI, the peak aspartate aminotransferase/alanine aminotransferase ratio and the maximum altered alkaline phosphatase or gamma-glutamyl transferase.Results: The final analysis comprised 183 cases in the experiment group and 187 cases in the control group. The risk of developing probable ATLI was not significantly different between the two groups. During the follow-up period, 43.72% of cases in the experiment group and 35.83% of cases in the control group were determined to have possible ATLI (relative risk = 1.23, 95% confidence interval: 0.94-1.54). When using a more strict definition of possible ATLI, the adjusted relative risk (95% confidence interval) was 1.76 (1.14-2.56). The risks of adverse drug reactions, prolonged treatment length, taking second-line tuberculosis drugs, and the clearance of tuberculosis bacteria were similar between the two groups. Conclusions: No significant preventive effect of silymarin was found for either lowering the risk of liver injury or boosting the positive outcomes. Worse, we even found a potential risk of liver damage caused by the hepatoprotectant.

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“…There are currently a number of challenges and controversies in exploiting predictive preclinical studies, especially for animal models, where ethical issues pose important limitations [20] .…”

Section: Issues In Drug Developmentmentioning

confidence: 99%

Assessing liver injury associated with antimycotics: Concise literature review and clues from data mining of the FAERS database

Raschi¹,

Poluzzi²,

Koci³

et al. 2014

WJH

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AIM: To inform clinicians on the level of hepatotoxic risk among antimycotics in the post-marketing setting, following the marketing suspension of oral ketoconazole for drug-induced liver injury (DILI). METHODS:The publicly available international FAERS database (2004)(2005)(2006)(2007)(2008)(2009)(2010)(2011) was used to extract DILI cases (including acute liver failure events), where antimycotics with systemic use or potential systemic absorption were reported as suspect or interacting agents. The reporting pattern was analyzed by calculating the reporting odds ratio and corresponding 95%CI, a measure of disproportionality, with time-trend analysis where appropriate. RESULTS:From 1687284 reports submitted over the 8-year period, 68115 regarded liver injury. Of these, 2.9% are related to antimycotics (1964 cases, of which 112 of acute liver failure). Eleven systemic antimycotics (including ketoconazole and the newer triazole derivatives voriconazole and posaconazole) and terbinafine (used systemically to treat onychomicosis) generated a significant disproportionality, indicating a post-marketing signal of risk. CONCLUSION:Virtually all antimycotics with systemic action or absorption are commonly reported in clinically significant cases of DILI. Clinicians must be aware of this aspect and monitor patients in case switch is considered, especially in critical poly-treated patients under chronic treatment.

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Current Challenges and Controversies in Drug-Induced Liver Injury

Cited by 54 publications

References 136 publications

High-Content Assays for Hepatotoxicity Using Induced Pluripotent Stem Cell–Derived Cells

High-Content Assays for Hepatotoxicity Using Induced Pluripotent Stem Cell–Derived Cells

Preventive use of a hepatoprotectant against anti‐tuberculosis drug‐induced liver injury: A randomized controlled trial

Assessing liver injury associated with antimycotics: Concise literature review and clues from data mining of the FAERS database

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