High Cardiomyocyte Diversity in Human Early Prenatal Heart Development

Overview

Journal iScience

Publisher Cell Press

Date 2023 Jan 10

PMID 36624836

Authors

Christer Sylven

Eva Wardell

Agneta Mansson-Broberg

Eugenio Cingolani

Konstantinos Ampatzis

Ludvig Larsson

Asa Bjorklund

Stefania Giacomello

Affiliations

Soon will be listed here.

Abstract

Cardiomyocytes play key roles during cardiogenesis, but have poorly understood features, especially in prenatal stages. Here, we characterized human prenatal cardiomyocytes, 6.5-7 weeks post-conception, by integrating single-cell RNA sequencing, spatial transcriptomics, and ligand-receptor interaction information. Using a computational workflow developed to dissect cell type heterogeneity, localize cell types, and explore their molecular interactions, we identified eight types of developing cardiomyocyte, more than double compared to the ones identified in the . These have high variability in cell cycle activity, mitochondrial content, and connexin gene expression, and are differentially distributed in the ventricles, including outflow tract, and atria, including sinoatrial node. Moreover, cardiomyocyte ligand-receptor crosstalk is mainly with non-cardiomyocyte cell types, encompassing cardiogenesis-related pathways. Thus, early prenatal human cardiomyocytes are highly heterogeneous and develop unique location-dependent properties, with complex ligand-receptor crosstalk. Further elucidation of their developmental dynamics may give rise to new therapies.

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