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Stress-free cell aggregation by using the CEPT cocktail enhances embryoid body and organoid fitness.

Seungmi RyuClaire MalleyPei-Hsuan ChuBen ErnestVukasin M JovanovicTao DengJaroslav SlameckaHyenjong HongYogita JethmalaniHannah M BaskirJason InmanJohn BraistedMarissa B HirstAnton SimeonovTy C VossCarlos A TristanIlyas Singeç
Published in: Biofabrication (2023)
Embryoid bodies (EBs) and self-organizing organoids derived from human pluripotent stem cells (hPSCs) recapitulate tissue development in a dish and hold great promise for disease modeling and drug development. However, current protocols are hampered by cellular stress and apoptosis during cell aggregation, resulting in variability and impaired cell differentiation. Here, we demonstrate that EBs and various organoid models (e.g., brain, gut, and kidney) can be optimized by using the CEPT small molecule cocktail, a polypharmacology approach that ensures cytoprotection and cell survival. Application of CEPT (chroman 1, emricasan, polyamine, trans-ISRIB) for just 24 hours during cell aggregation has long-lasting consequences affecting morphogenesis, gene expression, cellular differentiation, and function. Various qualification methods confirmed that CEPT treatment enhanced experimental reproducibility and consistently improved EB and organoid fitness as compared to the widely used ROCK inhibitor Y-27632. Collectively, we discovered that stress-free cell aggregation and superior cell survival in the presence of CEPT are critical quality control determinants that establish a robust foundation for bioengineering complex tissue and organ models.&#xD.
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