Characterization of liver zonation‐like transcriptomic patterns in <scp>HLCs</scp> derived from <scp>hiPSCs</scp> in a microfluidic biochip environment

Danoy, Mathieu; Poulain, Stéphane; Lereau-Bernier, Myriam; Kato, Sachi; Scheidecker, Benedikt; Kido, Taketomo; Miyajima, Atsushi; Sakai, Yasuyuki; Plessy, Charles; Leclerc, Éric

doi:10.1002/btpr.3013

Cited by 15 publications

(19 citation statements)

References 49 publications

(107 reference statements)

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“…The results showed hepatocyte polarity and the allowance of hepatobiliary function. In a later follow-up study, an oxygen measurement system was incorporated for toxicological screening [ 353 ]. In another study conducted by Lee et al, porcine liver dECM was used as bio-ink to print a 3D liver-on-a-chip platform.…”

Section: Engineered 3d In Vitro Modelsmentioning

confidence: 99%

Engineering Hydrogels for the Development of Three-Dimensional In Vitro Models

Maji

Lee

2022

IJMS

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The superiority of in vitro 3D cultures over conventional 2D cell cultures is well recognized by the scientific community for its relevance in mimicking the native tissue architecture and functionality. The recent paradigm shift in the field of tissue engineering toward the development of 3D in vitro models can be realized with its myriad of applications, including drug screening, developing alternative diagnostics, and regenerative medicine. Hydrogels are considered the most suitable biomaterial for developing an in vitro model owing to their similarity in features to the extracellular microenvironment of native tissue. In this review article, recent progress in the use of hydrogel-based biomaterial for the development of 3D in vitro biomimetic tissue models is highlighted. Discussions of hydrogel sources and the latest hybrid system with different combinations of biopolymers are also presented. The hydrogel crosslinking mechanism and design consideration are summarized, followed by different types of available hydrogel module systems along with recent microfabrication technologies. We also present the latest developments in engineering hydrogel-based 3D in vitro models targeting specific tissues. Finally, we discuss the challenges surrounding current in vitro platforms and 3D models in the light of future perspectives for an improved biomimetic in vitro organ system.

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Section: Engineered 3d In Vitro Modelsmentioning

confidence: 99%

Engineering Hydrogels for the Development of Three-Dimensional In Vitro Models

Maji

Lee

2022

IJMS

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“…In those optimized conditions, the tissue was still found to be positive to AFP and to CK19, and the mRNA levels of mature markers such as ALB and CYP3A4 were not found to reach the levels observed in Liver Total RNA samples. While the transcriptomics analysis of the comparison with Total Liver RNA samples as a positive control highlighted remaining patterns of primitiveness in the hiPSCs‐derived tissue (Figure S3), the current protocol has allowed detecting a CYP3A4 activity as well as an improved activity of several cytochromes over Petri dishes and over previously published protocols using biochips (Danoy et al, 2019, 2020). The multi‐omics analysis performed in the biochips revealed a signature, typical of a liver regenerative process, illustrated in Figures 5 and S4.…”

Section: Discussionmentioning

confidence: 81%

“…In this study, we present an extended maturation of hiPSCs‐derived HLCs in microfluidic biochip for 14 days under perfusion and stimulation with OSM. In addition, as we observed that the 5‐cm‐long microfluidic biochip that was used in our previous experiment would lead to a largely hypoxic culture condition (Danoy et al, 2020), we decided to shorten the microfluidic biochip to 1 cm. This design has shown its suitability for primary liver human hepatic cultures (Jellali et al, 2016) and allows the reduction of the required number of inoculated cells, which make it more suitable for larger‐scale experiments.…”

Section: Introductionmentioning

confidence: 99%

Multi‐omics analysis of hiPSCs‐derived HLCs matured on‐chip revealed patterns typical of liver regeneration

Danoy

Tauran

Poulain

et al. 2021

Biotech & Bioengineering

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Maturation of human‐induced pluripotent stem cells (hiPSCs)‐derived hepatocytes‐like cells (HLCs) toward a complete hepatocyte phenotype remains a challenge as primitiveness patterns are still commonly observed. In this study, we propose a modified differentiation protocol for those cells which includes a prematuration in Petri dishes and a maturation in microfluidic biochip. For the first time, a large range of biomolecular families has been extracted from the same sample to combine transcriptomic, proteomic, and metabolomic analysis. After integration, these datasets revealed specific molecular patterns and highlighted the hepatic regeneration profile in biochips. Overall, biochips exhibited processes of cell proliferation and inflammation (via TGFB1) coupled with anti‐fibrotic signaling (via angiotensin 1‐7, ATR‐2, and MASR). Moreover, cultures in this condition displayed physiological lipid‐carbohydrate homeostasis (notably via PPAR, cholesterol metabolism, and bile synthesis) coupled with cell respiration through advanced oxidative phosphorylation (through the overexpression of proteins from the third and fourth complex). The results presented provide an original overview of the complex mechanisms involved in liver regeneration using an advanced in vitro organ‐on‐chip technology.

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“…Indeed, as cells are injected in biochips at a progenitor stage, they still retain part of their pluripotency which allows them to differentiate toward a different lineage in the biochip. Especially, the presence of endothelial-like cells and hypoxia-related phenotypes was confirmed in longer biochips after 7 days of maturation ( Danoy et al , 2019 , Danoy et al , 2020b ). In the current setup, the length of the biochip was reduced by 5 folds and hypoxia-related phenotype was not highlighted.…”

Section: Discussionmentioning

confidence: 86%

Investigation of the hepatic development in the coculture of hiPSCs-derived LSECs and HLCs in a fluidic microenvironment

Danoy

Tauran

Poulain³

et al. 2021

APL Bioengineering

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Interactions between the different liver cell types are critical to the maintenance or induction of their function in vitro . In this work, human-induced Pluripotent Stem Cells (hiPSCs)-derived Liver Sinusoidal Endothelial Cells (LSECs) and Hepatocytes-Like Cells (HLCs) were cultured and matured in a microfluidic environment. Both cell populations were differentiated in Petri dishes, detached, and inoculated in microfluidic biochips. In cocultures of both cell types, the tissue has exhibited a higher production of albumin (3.19 vs 5.31 μ g/mL/10 6 cells in monocultures and cocultures) as well as a higher inducibility CYP450 over monocultures of HLCs. Tubular-like structures composed of LSECs and positive for the endothelial marker PECAM1, as well as a tissue more largely expressing Stabilin-2 were detected in cocultures only. In contrast, monocultures exhibited no network and less specific endothelial markers. The transcriptomic analysis did not reveal a marked difference between the profiles of both culture conditions. Nevertheless, the analysis allowed us to highlight different upstream regulators in cocultures (SP1, EBF1, and GATA3) and monocultures (PML, MECP2, and NRF1). In cocultures, the multi-omics dataset after 14 days of maturation in biochips has shown the activation of signaling related to hepatic maturation, angiogenesis, and tissue repair. In this condition, inflammatory signaling was also found to be reduced when compared to monocultures as illustrated by the activation of NFKB and by the detection of several cytokines involved in tissue injury in the latter. Finally, the extracted biological processes were discussed regarding the future development of a new generation of human in vitro hepatic models.

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Characterization of liver zonation‐like transcriptomic patterns in HLCs derived from hiPSCs in a microfluidic biochip environment

Cited by 15 publications

References 49 publications

Engineering Hydrogels for the Development of Three-Dimensional In Vitro Models

Engineering Hydrogels for the Development of Three-Dimensional In Vitro Models

Multi‐omics analysis of hiPSCs‐derived HLCs matured on‐chip revealed patterns typical of liver regeneration

Investigation of the hepatic development in the coculture of hiPSCs-derived LSECs and HLCs in a fluidic microenvironment

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