Author: Litviňuková, Monika; Talavera-López, Carlos; Maatz, Henrike; Reichart, Daniel; Worth, Catherine L.; Lindberg, Eric L.; Kanda, Masatoshi; Polanski, Krzysztof; Heinig, Matthias; Lee, Michael; Nadelmann, Emily R.; Roberts, Kenny; Tuck, Liz; Fasouli, Eirini S.; DeLaughter, Daniel M.; McDonough, Barbara; Wakimoto, Hiroko; Gorham, Joshua M.; Samari, Sara; Mahbubani, Krishnaa T.; Saeb-Parsy, Kourosh; Patone, Giannino; Boyle, Joseph J.; Zhang, Hongbo; Zhang, Hao; Viveiros, Anissa; Oudit, Gavin Y.; Bayraktar, Omer Ali; Seidman, J. G.; Seidman, Christine E.; Noseda, Michela; Hubner, Norbert; Teichmann, Sarah A.
Title: Cells of the adult human heart Cord-id: bq1q265y Document date: 2020_9_24
ID: bq1q265y
Snippet: Cardiovascular disease is the leading cause of death worldwide. Advanced insights into disease mechanisms and therapeutic strategies require a deeper understanding of the molecular processes involved in the healthy heart. Knowledge of the full repertoire of cardiac cells and their gene expression profiles is a fundamental first step in this endeavour. Here, using state-of-the-art analyses of large-scale single-cell and single-nucleus transcriptomes, we characterize six anatomical adult heart reg
Document: Cardiovascular disease is the leading cause of death worldwide. Advanced insights into disease mechanisms and therapeutic strategies require a deeper understanding of the molecular processes involved in the healthy heart. Knowledge of the full repertoire of cardiac cells and their gene expression profiles is a fundamental first step in this endeavour. Here, using state-of-the-art analyses of large-scale single-cell and single-nucleus transcriptomes, we characterize six anatomical adult heart regions. Our results highlight the cellular heterogeneity of cardiomyocytes, pericytes and fibroblasts, and reveal distinct atrial and ventricular subsets of cells with diverse developmental origins and specialized properties. We define the complexity of the cardiac vasculature and its changes along the arterio-venous axis. In the immune compartment, we identify cardiac-resident macrophages with inflammatory and protective transcriptional signatures. Furthermore, analyses of cell-to-cell interactions highlight different networks of macrophages, fibroblasts and cardiomyocytes between atria and ventricles that are distinct from those of skeletal muscle. Our human cardiac cell atlas improves our understanding of the human heart and provides a valuable reference for future studies.
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