Microscale Collagen and Fibroblast Interactions Enhance Primary Human Hepatocyte Functions in Three-Dimensional Models

Kukla, David A.; Crampton, Alexandra L.; Wood, David K.; Khetani, Salman R.

doi:10.3727/105221620x15868728381608

Cited by 22 publications

(34 citation statements)

References 43 publications

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“…Those spheroids, often called microtissues, displayed pronounced glycogen storage and albumin synthesis capabilities as well as expression of CYP1A2, CYP2C9 and CYP3A4. Maintenance of cell polarity could be shown by MRP2 and BSEP expression [ 64 , 65 , 66 ]. Viability of the spheroids could be maintained for up to 7 weeks in one of the studies, but albumin secretion declined from day 28 on.…”

Section: Three-dimensional Culture Models For Human Hepatocytesmentioning

confidence: 99%

“…Viability of the spheroids could be maintained for up to 7 weeks in one of the studies, but albumin secretion declined from day 28 on. Interestingly, CYP1A1/2 , CYP2C9 and CYP3A4/5 transcript levels were higher in those microtissues than in clinical liver specimens or pHHs upon long-term culture [ 65 , 66 ]. However, on protein level, only CYP2B6 and UGT1A1 levels remained stable for 7 weeks of culture.…”

Section: Three-dimensional Culture Models For Human Hepatocytesmentioning

confidence: 99%

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Three-Dimensional Liver Culture Systems to Maintain Primary Hepatic Properties for Toxicological Analysis In Vitro

Kammerer

2021

IJMS

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Drug-induced liver injury (DILI) is the major reason for failures in drug development and withdrawal of approved drugs from the market. Two-dimensional cultures of hepatocytes often fail to reliably predict DILI: hepatoma cell lines such as HepG2 do not reflect important primary-like hepatic properties and primary human hepatocytes (pHHs) dedifferentiate quickly in vitro and are, therefore, not suitable for long-term toxicity studies. More predictive liver in vitro models are urgently required in drug development and compound safety evaluation. This review discusses available human hepatic cell types for in vitro toxicology analysis and their usage in established and emerging three-dimensional (3D) culture systems. Generally, 3D cultures maintain or improve primary hepatic functions (including expression of drug-metabolizing enzymes) of different liver cells for several weeks of culture, thus allowing long-term and repeated-dose toxicity studies. Spheroid cultures of pHHs have been comprehensively tested, but also other cell types such as HepaRG benefit from 3D culture systems. Emerging 3D culture techniques include usage of induced pluripotent stem-cell-derived hepatocytes and primary-like upcyte cells, as well as advanced culture techniques such as microfluidic liver-on-a-chip models. In-depth characterization of existing and emerging 3D hepatocyte technologies is indispensable for successful implementation of such systems in toxicological analysis.

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Section: Three-dimensional Culture Models For Human Hepatocytesmentioning

confidence: 99%

Section: Three-dimensional Culture Models For Human Hepatocytesmentioning

confidence: 99%

Three-Dimensional Liver Culture Systems to Maintain Primary Hepatic Properties for Toxicological Analysis In Vitro

Kammerer

2021

IJMS

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“…(f) A high-throughput droplet microfluidic device for the generation of 3D liver microtissues. 85 Left to right: Hepatocytes are suspended in collagen solution and perfused through the microfluidic device at 4 °C (to keep collagen from polymerizing) with an oil stream; since oil and water do not mix, the collagen + cells form spherical droplets. These so-called microtissues are collected, heated at 37 °C to promote collagen polymerization and cell encapsulation, oil is drained, and microtissues are resuspended in culture medium within microwells in static or fluidic plates/devices.…”

Section: Engineered Human Liver Models Validated For Drug Testingmentioning

confidence: 99%

“…For instance, a high-throughput droplet microfluidic technology was used to encapsulate PHHs within ECM microgels, which were subsequently “coated” with 3T3-J2 fibroblasts or HSCs [ Fig. 3(f) ]; 85 the PHH/fibroblast “microtissues” displayed high levels of liver functions for 6+ weeks in vitro and functionally outperformed self-assembled spheroids and macrogels of the same cellular composition. These microtissues displayed clinically relevant CYP induction with prototypical compounds and could distinguish troglitazone toxicity from that of its non-hepatotoxic structural analog drug, rosiglitazone.…”

Section: Engineered Human Liver Models Validated For Drug Testingmentioning

confidence: 99%

Latest impact of engineered human liver platforms on drug development

2021

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Drug-induced liver injury (DILI) is a leading cause of drug attrition, which is partly due to differences between preclinical animals and humans in metabolic pathways. Therefore, in vitro human liver models are utilized in biopharmaceutical practice to mitigate DILI risk and assess related mechanisms of drug transport and metabolism. However, liver cells lose phenotypic functions within 1–3 days in two-dimensional monocultures on collagen-coated polystyrene/glass, which precludes their use to model the chronic effects of drugs and disease stimuli. To mitigate such a limitation, bioengineers have adapted tools from the semiconductor industry and additive manufacturing to precisely control the microenvironment of liver cells. Such tools have led to the fabrication of advanced two-dimensional and three-dimensional human liver platforms for different throughput needs and assay endpoints (e.g., micropatterned cocultures, spheroids, organoids, bioprinted tissues, and microfluidic devices); such platforms have significantly enhanced liver functions closer to physiologic levels and improved functional lifetime to >4 weeks, which has translated to higher sensitivity for predicting drug outcomes and enabling modeling of diseased phenotypes for novel drug discovery. Here, we focus on commercialized engineered liver platforms and case studies from the biopharmaceutical industry showcasing their impact on drug development. We also discuss emerging multi-organ microfluidic devices containing a liver compartment that allow modeling of inter-tissue crosstalk following drug exposure. Finally, we end with key requirements for engineered liver platforms to become routine fixtures in the biopharmaceutical industry toward reducing animal usage and providing patients with safe and efficacious drugs with unprecedented speed and reduced cost.

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“…Therefore, in a recent study, high-throughput droplet microfluidics was utilized to generate uniform microtissues with PHHs encapsulated in collagen I with supportive fibroblasts (3T3-J2 or HSC). 71 These microtissues displayed high hepatic functions for 6þ weeks and were found to be useful for assessing drugmediated cytochrome-P450 (CYP) induction and hepatotoxicity. Such microtissues are now being adapted to include other liver cell types and to study the pathogenesis of diseases such as NAFLD and fibrosis.…”

Section: D-printed Organoids and Tissuesmentioning

confidence: 99%

Bioengineered Liver Models for Investigating Disease Pathogenesis and Regenerative Medicine

Kukla

Khetani

2021

Semin Liver Dis

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Owing to species-specific differences in liver pathways, in vitro human liver models are utilized for elucidating mechanisms underlying disease pathogenesis, drug development, and regenerative medicine. To mitigate limitations with de-differentiated cultures, bioengineers have developed advanced techniques/platforms, including micropatterned cocultures, spheroids/organoids, bioprinting, and microfluidic devices, for perfusing cell cultures and liver slices. Such techniques improve mature functions and culture lifetime of primary and stem-cell human liver cells. Furthermore, bioengineered liver models display several features of liver diseases including infections with pathogens (e.g., malaria, hepatitis C/B viruses, Zika, dengue, yellow fever), alcoholic/nonalcoholic fatty liver disease, and cancer. Here, we discuss features of bioengineered human liver models, their uses for modeling aforementioned diseases, and how such models are being augmented/adapted for fabricating implantable human liver tissues for clinical therapy. Ultimately, continued advances in bioengineered human liver models have the potential to aid the development of novel, safe, and efficacious therapies for liver disease.

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Microscale Collagen and Fibroblast Interactions Enhance Primary Human Hepatocyte Functions in Three-Dimensional Models

Cited by 22 publications

References 43 publications

Three-Dimensional Liver Culture Systems to Maintain Primary Hepatic Properties for Toxicological Analysis In Vitro

Three-Dimensional Liver Culture Systems to Maintain Primary Hepatic Properties for Toxicological Analysis In Vitro

Latest impact of engineered human liver platforms on drug development

Bioengineered Liver Models for Investigating Disease Pathogenesis and Regenerative Medicine

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