| Literature DB >> 34019794 |
Pablo Hofbauer1, Stefan M Jahnel1, Nora Papai1, Magdalena Giesshammer1, Alison Deyett1, Clara Schmidt1, Mirjam Penc1, Katherina Tavernini1, Nastasja Grdseloff1, Christy Meledeth1, Lavinia Ceci Ginistrelli1, Claudia Ctortecka1, Šejla Šalic1, Maria Novatchkova2, Sasha Mendjan3.
Abstract
Organoids capable of forming tissue-like structures have transformed our ability to model human development and disease. With the notable exception of the human heart, lineage-specific self-organizing organoids have been reported for all major organs. Here, we established self-organizing cardioids from human pluripotent stem cells that intrinsically specify, pattern, and morph into chamber-like structures containing a cavity. Cardioid complexity can be controlled by signaling that instructs the separation of cardiomyocyte and endothelial layers and by directing epicardial spreading, inward migration, and differentiation. We find that cavity morphogenesis is governed by a mesodermal WNT-BMP signaling axis and requires its target HAND1, a transcription factor linked to developmental heart chamber defects. Upon cryoinjury, cardioids initiated a cell-type-dependent accumulation of extracellular matrix, an early hallmark of both regeneration and heart disease. Thus, human cardioids represent a powerful platform to mechanistically dissect self-organization, congenital heart defects and serve as a foundation for future translational research.Entities:
Keywords: cardiac injury model; cardiac organoid; cardioids; congenital heart defects; heart development; heart organoid; human pluripotent stem cells; mesoderm; self-organization; self-organizing organoids
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Year: 2021 PMID: 34019794 DOI: 10.1016/j.cell.2021.04.034
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582