Spatial transcriptomics reveals a key role of fibroblast-like vascular smooth muscle cells in human atherosclerotic cell crosstalk and stability
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Peer-reviewed
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Abstract
Abstract
Background and Aims
Atherosclerotic plaques are the leading cause of cardiovascular events. Single-cell approaches have identified diverse human plaque cell phenotypes but their spatial distribution and interactions remain unclear. Here, intercellular communication patterns in human plaque microenvironments were mapped to reveal novel targets to prevent atherosclerotic events.
Methods
Spatial transcriptomics (Visium, 10x) from 13 carotid plaques, and single-cell transcriptomics (cells = 51 981) were used to analyse cell phenotypes, cell trajectories, and intercellular communications. Cells contributing to plaque stability were explored using deconvolution of plaque bulk RNA-seq data (n = 78), histology, and survival analyses. Key cells and pathways were validated in apolipoprotein E (Apoe)−/− mice and in vitro. Genome-wide association study enrichment analyses were conducted using summary statistics of atherosclerotic diseases. LINCS L1000 data were used to explore drug repurposing.
Results
A fibroblast-like vascular smooth muscle cell (VSMC) phenotype associated with extracellular matrix formation pathways (validated in Apoe−/− mice) emerged as a key regulator of intra-plaque ligand-receptor signalling, in particular in the cap region. A higher proportion of fibroblast-like VSMCs was found in asymptomatics, associated with stable plaque features and predicted a lower risk of future events. Genes specific to this VSMC phenotype were enriched in coronary artery disease and myocardial infarction. Finally, compounds, which could induce key marker genes were identified and validated in vitro.
Conclusions
This study provides the first comprehensive spatial transcriptomics map of cell communication in human plaque microenvironments. A pivotal role of a fibroblast-like VSMC, orchestrating intraplaque cell signalling and contributing to plaque stability, was identified. Targeting these cells might present promising novel avenues for therapies.
Description
Acknowledgements: We thank Dr Mohammad Barghouth for his technical support.
Funder: Skåne University hospital; doi: https://doi.org/10.13039/501100011077
Funder: Lund University Diabetes Center
Funder: Bundy Academy; doi: https://doi.org/10.13039/501100021728
Funder: Knut and Alice Wallenberg foundation; doi: https://doi.org/10.13039/501100004063
Funder: Lund University and Region Skåne
Journal Title
European Heart Journal
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0195-668X
1522-9645
1522-9645
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Oxford University Press (OUP)
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Except where otherwised noted, this item's license is described as https://creativecommons.org/licenses/by/4.0/
Sponsorship
Swedish Society for Medical Research (CG-22-0254-H-02)
Swedish Research Council (2019-01260, 2023-02368, 2019-01907, 2024-02761, 2009-1039)
Swedish Heart Lung Foundation (20220044, 20220284, 20240143, 20200403, 20230257, 20241210)
Swedish Stroke Association (S-993166)
Swedish Foundation for Strategic Research (Dnr IRC15-0067)
LeDucq Foundation Network of Excellence (22CVD02)
Swedish Research Council (2019-01260, 2023-02368, 2019-01907, 2024-02761, 2009-1039)
Swedish Heart Lung Foundation (20220044, 20220284, 20240143, 20200403, 20230257, 20241210)
Swedish Stroke Association (S-993166)
Swedish Foundation for Strategic Research (Dnr IRC15-0067)
LeDucq Foundation Network of Excellence (22CVD02)