Publications by authors named "Teresa Izuel-Idoype"

Terminally differentiated cells are commonly regarded as the most stable cell state in adult organisms, characterized by growth arrest while fulfilling their specialized functions. A better understanding of the mechanisms involved in promoting cell cycle exit will improve the ability to differentiate pluripotent cells into mature tissues for both pharmacological and therapeutic use. Here, it demonstrates that a hyperosmolar environment enforces a protective p53-independent quiescent state in immature hepatoma cells and in pluripotent stem cell-derived models of human hepatocytes and endothelial cells.

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Article Synopsis
  • Human pluripotent stem cell-derived hepatocyte-like cells (HLCs) are promising for liver disease studies, drug testing, and toxicity evaluations but face challenges like high production costs and complex differentiation processes.
  • An automated liquid handling system was used in the differentiation of HLCs, significantly reducing costs by about 79% and allowing for the screening of cheaper alternatives to growth factors.
  • The study found that using a combination of small molecules and Laminin-521 produced HLCs with similar characteristics and functionality to those made with traditional growth factors, enabling a scalable and cost-effective method for HLC production.
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Chronic liver injury, as observed in non-alcoholic steatohepatitis (NASH), progressive fibrosis, and cirrhosis, remains poorly treatable. Steatohepatitis causes hepatocyte loss in part by a direct lipotoxic insult, which is amplified by derangements in the non-parenchymal cellular (NPC) interactive network wherein hepatocytes reside, including, hepatic stellate cells, liver sinusoidal endothelial cells and liver macrophages. To create an in vitro culture model encompassing all these cells, that allows studying liver steatosis, inflammation and fibrosis caused by NASH, we here developed a fully defined hydrogel microenvironment, termed hepatocyte maturation (HepMat) gel, that supports maturation and maintenance of pluripotent stem cell (PSC) derived hepatocyte- and NPC-like cells for at least one month.

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