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Literature DB >> 24764241

In vitro platforms for evaluating liver toxicity.

Shyam Sundhar Bale¹, Lawrence Vernetti^2,3, Nina Senutovitch^2,3, Rohit Jindal¹, Manjunath Hegde¹, Albert Gough^2,3, William J McCarty¹, Ahmet Bakan³, Abhinav Bhushan¹, Tong Ying Shun², Inna Golberg¹, Richard DeBiasio², Berk Osman Usta¹, D Lansing Taylor^2,3, Martin L Yarmush¹.

Abstract

The liver is a heterogeneous organ with many vital functions, including metabolism of pharmaceutical drugs and is highly susceptible to injury from these substances. The etiology of drug-induced liver disease is still debated although generally regarded as a continuum between an activated immune response and hepatocyte metabolic dysfunction, most often resulting from an intermediate reactive metabolite. This debate stems from the fact that current animal and in vitro models provide limited physiologically relevant information, and their shortcomings have resulted in "silent" hepatotoxic drugs being introduced into clinical trials, garnering huge financial losses for drug companies through withdrawals and late stage clinical failures. As we advance our understanding into the molecular processes leading to liver injury, it is increasingly clear that (a) the pathologic lesion is not only due to liver parenchyma but is also due to the interactions between the hepatocytes and the resident liver immune cells, stellate cells, and endothelial cells; and (b) animal models do not reflect the human cell interactions. Therefore, a predictive human, in vitro model must address the interactions between the major human liver cell types and measure key determinants of injury such as the dosage and metabolism of the drug, the stress response, cholestatic effect, and the immune and fibrotic response. In this mini-review, we first discuss the current state of macro-scale in vitro liver culture systems with examples that have been commercialized. We then introduce the paradigm of microfluidic culture systems that aim to mimic the liver with physiologically relevant dimensions, cellular structure, perfusion, and mass transport by taking advantage of micro and nanofabrication technologies. We review the most prominent liver-on-a-chip platforms in terms of their physiological relevance and drug response. We conclude with a commentary on other critical advances such as the deployment of fluorescence-based biosensors to identify relevant toxicity pathways, as well as computational models to create a predictive tool.

Entities: CellLine Chemical Disease Gene Species

Keywords: Drug-induced liver injury; hepatotoxicity; high content screening; liver on chip; predictive modeling

Mesh：

Year: 2014 PMID： 24764241 PMCID： PMC4156546 DOI： 10.1177/1535370214531872

Source DB: PubMed Journal: Exp Biol Med (Maywood) ISSN： 1535-3699

110 in total

1. Genetically encoded fluorescent reporters of protein tyrosine kinase activities in living cells.

Authors: A Y Ting; K H Kain; R L Klemke; R Y Tsien
Journal: Proc Natl Acad Sci U S A Date: 2001-12-18 Impact factor: 11.205

2. Fluorescence-based assays for screening nine cytochrome P450 (P450) activities in intact cells expressing individual human P450 enzymes.

Authors: M Teresa Donato; Nuria Jiménez; José V Castell; M José Gómez-Lechón
Journal: Drug Metab Dispos Date: 2004-07 Impact factor: 3.922

3. Imaging dynamic redox changes in mammalian cells with green fluorescent protein indicators.

Authors: Colette T Dooley; Timothy M Dore; George T Hanson; W Coyt Jackson; S James Remington; Roger Y Tsien
Journal: J Biol Chem Date: 2004-02-25 Impact factor: 5.157

4. Microreactor microfluidic systems with human microsomes and hepatocytes for use in metabolite studies.

Authors: Jeanna C Zguris; Laura J Itle; Daniel Hayes; Michael V Pishko
Journal: Biomed Microdevices Date: 2005-06 Impact factor: 2.838

5. A single circularly permuted GFP sensor for inositol-1,3,4,5-tetrakisphosphate based on a split PH domain.

Authors: Reiko Sakaguchi; Takashi Endoh; Seigo Yamamoto; Kazuki Tainaka; Kenji Sugimoto; Nobutaka Fujieda; Shigeki Kiyonaka; Yasuo Mori; Takashi Morii
Journal: Bioorg Med Chem Date: 2009-08-13 Impact factor: 3.641

Review 6. The roles of MRP2, MRP3, OATP1B1, and OATP1B3 in conjugated hyperbilirubinemia.

Authors: Dietrich Keppler
Journal: Drug Metab Dispos Date: 2014-01-23 Impact factor: 3.922

7. Hepatocyte function and extracellular matrix geometry: long-term culture in a sandwich configuration.

Authors: J C Dunn; M L Yarmush; H G Koebe; R G Tompkins
Journal: FASEB J Date: 1989-02 Impact factor: 5.191

8. Correlation of biliary excretion in sandwich-cultured rat hepatocytes and in vivo in rats.

Authors: X Liu; J P Chism; E L LeCluyse; K R Brouwer; K L Brouwer
Journal: Drug Metab Dispos Date: 1999-06 Impact factor: 3.922

9. Microenvironmental regulation of the sinusoidal endothelial cell phenotype in vitro.

Authors: Sandra March; Elliot E Hui; Gregory H Underhill; Salman Khetani; Sangeeta N Bhatia
Journal: Hepatology Date: 2009-09 Impact factor: 17.425

10. Evaluation of a microfluidic based cell culture platform with primary human hepatocytes for the prediction of hepatic clearance in human.

Authors: P Chao; T Maguire; E Novik; K-C Cheng; M L Yarmush
Journal: Biochem Pharmacol Date: 2009-05-20 Impact factor: 5.858

46 in total

In vitro platforms for evaluating liver toxicity.

1. Genetically encoded fluorescent reporters of protein tyrosine kinase activities in living cells.

2. Fluorescence-based assays for screening nine cytochrome P450 (P450) activities in intact cells expressing individual human P450 enzymes.

3. Imaging dynamic redox changes in mammalian cells with green fluorescent protein indicators.

4. Microreactor microfluidic systems with human microsomes and hepatocytes for use in metabolite studies.

5. A single circularly permuted GFP sensor for inositol-1,3,4,5-tetrakisphosphate based on a split PH domain.

Review 6. The roles of MRP2, MRP3, OATP1B1, and OATP1B3 in conjugated hyperbilirubinemia.

7. Hepatocyte function and extracellular matrix geometry: long-term culture in a sandwich configuration.

8. Correlation of biliary excretion in sandwich-cultured rat hepatocytes and in vivo in rats.

9. Microenvironmental regulation of the sinusoidal endothelial cell phenotype in vitro.

10. Evaluation of a microfluidic based cell culture platform with primary human hepatocytes for the prediction of hepatic clearance in human.

Review 1. Liver metastases: Microenvironments and ex-vivo models.

2. Towards engineering integrated cardiac organoids: beating recorded.

Review 3. Opportunities and challenges in the wider adoption of liver and interconnected microphysiological systems.

Review 4. Fluorescent protein biosensors applied to microphysiological systems.

5. A novel low-volume two-chamber microfabricated platform for evaluating drug metabolism and toxicity.

6. Long-term coculture strategies for primary hepatocytes and liver sinusoidal endothelial cells.

7. Biology coming full circle: joining the whole and the parts.

Review 8. Emerging In Vitro Liver Technologies for Drug Metabolism and Inter-Organ Interactions.

9. Long-term maintenance of a microfluidic 3D human liver sinusoid.

Review 10. Liver and Kidney on Chips: Microphysiological Models to Understand Transporter Function.