Abstract 16742: Single-Cell Transcriptional and Epigenomic Dissection of Human Heart in Health and Coronary Artery Disease Reveals Cell-type-Specific Driver Genes and Pathways

Kuosmanen, Suvi Linna; Schmauch, Eloi; Galani, Kyriaki; Boix, Carles; Park, Yongjin P.; Hollmén, Maija; Gunn, Jarmo; Kiviniemi, Tuomas; García‐Cardeña, Guillermo; Kellis, M

doi:10.1161/circ.142.suppl_3.16742

Cited by 1 publication

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“…Moreover, clinical trials showed benefit for Canakinumab in heart failure, suggesting a causal role for IL-1β in its pathogenesis 106 . Although recent studies pointed to cytokine-mediated fibroblast activation 107 and expansion of stressed CMs in ischemia 108 , the precise cellular mechanisms responsible for fibroblast activation or CM transition to a stressed status remains unclear. Our finding of inflammatory cytokine receptor expression in the vCM3_stressed cells provides a potential mechanism mediating CM susceptibility to inflammation, remodelling, and death.…”

Section: Discussionmentioning

confidence: 99%

Spatially resolved multiomics of human cardiac niches

Kanemaru¹,

Cranley²,

Muraro³

et al. 2023

Preprint

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A cell's function is defined by its intrinsic characteristics and its niche: the tissue microenvironment in which it dwells. Here, we combine single-cell and spatial transcriptomic data to discover cellular niches within eight regions of the human heart. We map cells to micro-anatomic locations and integrate knowledge-based and unsupervised structural annotations. For the first time, we profile the cells of the human cardiac conduction system, revealing their distinctive repertoire of ion channels, G-protein coupled receptors, and cell interactions using a custom CellPhoneDB.org module. We show that the sinoatrial node is compartmentalised, with a core of pacemaker cells, fibroblasts and glial cells supporting paracrine glutamatergic signalling. We introduce a druggable target prediction tool, drug2cell, which leverages single-cell profiles and drug-target interactions, providing unexpected mechanistic insights into the chronotropic effects of drugs, including GLP-1 analogues. In the epicardium, we show enrichment of both IgG+ and IgA+ plasma cells forming immune niches which may contribute to infection defence. We define a ventricular myocardial-stress niche enriched for activated fibroblasts and stressed cardiomyocytes, cell states that are expanded in cardiomyopathies. Overall, we provide new clarity to cardiac electro-anatomy and immunology, and our suite of computational approaches can be deployed to other tissues and organs.

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Section: Discussionmentioning

confidence: 99%