A single-cell comparison of adult and fetal human epicardium defines the age-associated changes in epicardial activity

Author:

Knight-Schrijver Vincent R.ORCID,Davaapil Hongorzul,Bayraktar Semih,Ross Alexander D. B.,Kanemaru Kazumasa,Cranley James,Dabrowska Monika,Patel Minal,Polanski Krzysztof,He Xiaoling,Vallier Ludovic,Teichmann Sarah,Gambardella LaureORCID,Sinha SanjayORCID

Abstract

AbstractRe-activating quiescent adult epicardium represents a potential therapeutic approach for human cardiac regeneration. However, the exact molecular differences between inactive adult and active fetal epicardium are not known. In this study, we combined fetal and adult human hearts using single-cell and single-nuclei RNA sequencing and compared epicardial cells from both stages. We found that a migratory fibroblast-like epicardial population only in the fetal heart and fetal epicardium expressed angiogenic gene programs, whereas the adult epicardium was solely mesothelial and immune responsive. Furthermore, we predicted that adult hearts may still receive fetal epicardial paracrine communication, including WNT signaling with endocardium, reinforcing the validity of regenerative strategies that administer or reactivate epicardial cells in situ. Finally, we explained graft efficacy of our human embryonic stem-cell-derived epicardium model by noting its similarity to human fetal epicardium. Overall, our study defines epicardial programs of regenerative angiogenesis absent in adult hearts, contextualizes animal studies and defines epicardial states required for effective human heart regeneration.

Funder

BHF Centre of Research Excellence, Oxford

Wellcome Trust

British Heart Foundation

Takeda Science Foundation

Wellcome Trust Clinical PhD Fellowship

Publisher

Springer Science and Business Media LLC

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