2019
DOI: 10.1186/s13287-019-1367-x
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Adult and iPS-derived non-parenchymal cells regulate liver organoid development through differential modulation of Wnt and TGF-β

Abstract: Background: Liver organoid technology holds great promises to be used in large-scale population-based drug screening and in future regenerative medicine strategies. Recently, some studies reported robust protocols for generating isogenic liver organoids using liver parenchymal and non-parenchymal cells derived from induced pluripotent stem cells (iPS) or using isogenic adult primary non-parenchymal cells. However, the use of whole iPSderived cells could represent great challenges for a translational perspectiv… Show more

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Cited by 42 publications
(39 citation statements)
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“…Proteomic analysis of four different types of hPSC-LBs (HAEC/dpMSCs; HAEC/hPSC-derived MSCs; hPSC-derived ECs/dpMSCs and entirely hPSC-derived LB) revealed differences in the WNT and TGF-β pathways among the four groups. The high TGF-β expression in HAECs was related to impaired hepatocyte differentiation from hepatoblasts as shown by a decrease in hPSC-LB albumin production, which was probably caused by remodeling of the ECM [73]. In accordance with this, Koui et al showed that hPSC-derived LSECs and hPSC-derived MSCs improved expansion, maintenance and metabolic rate of hPSC-derived hepatocytes compared to that of their primary counterparts (HUVECs and MSCs) in a 2D-coculture [74].…”
Section: Liver Organoids and Vascularizationmentioning
confidence: 84%
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“…Proteomic analysis of four different types of hPSC-LBs (HAEC/dpMSCs; HAEC/hPSC-derived MSCs; hPSC-derived ECs/dpMSCs and entirely hPSC-derived LB) revealed differences in the WNT and TGF-β pathways among the four groups. The high TGF-β expression in HAECs was related to impaired hepatocyte differentiation from hepatoblasts as shown by a decrease in hPSC-LB albumin production, which was probably caused by remodeling of the ECM [73]. In accordance with this, Koui et al showed that hPSC-derived LSECs and hPSC-derived MSCs improved expansion, maintenance and metabolic rate of hPSC-derived hepatocytes compared to that of their primary counterparts (HUVECs and MSCs) in a 2D-coculture [74].…”
Section: Liver Organoids and Vascularizationmentioning
confidence: 84%
“…Other approaches attempting to vascularize LBs have been based on the use of human adipose microvascular endothelial cells (HAMECs) as a source of human ECs [70]. Recently, some studies have succeeded in generating LBs entirely from hPSCs by either a codifferentiation approach [71] or an independent differentiation of hPSCs into ECs, MSCs and hepatoblasts and their subsequent coculture [72][73][74]. Similar to HUVECs and HAMECs, hPSC-derived ECs have been shown to improve the maturation of hepatocytes and the engraftment of hPSC-hepatocytes in in vivo models (Ramanathan et al 2015) [70][71][72]75].…”
Section: Liver Organoids and Vascularizationmentioning
confidence: 99%
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“…hiPSCs were differentiated toward definitive endoderm (DE) according to Goulart et al 26 with minor modifications. hiPSC cells were seeded at 2.5 × 104 cells/cm 2 on GELTREX coated plates and cultured for 3 days until reached 40% confluency.…”
Section: Methodsmentioning
confidence: 99%
“…41,52,154 Initial studies focusing on differentiation and maturation of iPSC-hepatocytes in 3D systems yielded promising results for obtaining functional and gene expression profiles that are closer to the activity of primary tissues. [155][156][157] However, in addition to better investigating the mechanistic implications of 3D microenvironments in iPSChepatocyte differentiation, the potential employment of these systems with differentiated cells for drug clearance studies still requires elucidation. Once validated for this context, engineered systems with iPSC-differentiated cells will provide the opportunity of replicating patient-specific properties that relate to the expression of enzymes and transporters.…”
Section: Toxicitymentioning
confidence: 99%