Multi-chamber cardioids unravel human heart development and cardiac defects

Clara Schmidt(Institute of Molecular Biotechnology), Alison Deyett(Institute of Molecular Biotechnology), Tobias Ilmer(Institute of Molecular Biotechnology), Aranxa Torres Caballero(Institute of Molecular Biotechnology), Simon Haendeler(Max Perutz Labs), Lokesh G. Pimpale, Michael A. Netzer(University of Vienna), Lavinia Ceci Ginistrelli(Institute of Molecular Biotechnology), Martina Cirigliano(Institute of Molecular Biotechnology), Estela Juncosa Mancheno(Institute of Molecular Biotechnology), Daniel Reumann(Institute of Molecular Biotechnology), Katherina Tavernini(Institute of Molecular Biotechnology), Steffen Hering(University of Vienna), Pablo Hofbauer, Sasha Mendjan(Institute of Molecular Biotechnology)
bioRxiv (Cold Spring Harbor Laboratory)
July 16, 2022
Cited by 14Open Access
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Abstract

The number one cause of human fetal death are defects in heart development. Because the human embryonic heart is inaccessible, and the impacts of mutations, drugs, and environmental factors on the specialized functions of different heart compartments are not captured by in vitro models, determining the underlying causes is difficult. Here, we established a human cardioid platform that recapitulates the development of all major embryonic heart compartments, including right and left ventricles, atria, outflow tract, and atrioventricular canal. By leveraging both 2D and 3D differentiation, we efficiently generated progenitor subsets with distinct first, anterior, and posterior second heart field identities. This advance enabled the reproducible generation of cardioids with compartment-specific in vivo-like gene expression profiles, morphologies, and functions. We used this platform to unravel the ontogeny of signal and contraction propagation between interacting heart chambers and dissect how genetic and environmental factors cause region-specific defects in the developing human heart.


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