4.8 Article

Origin and function of activated fibroblast states during zebrafish heart regeneration

Journal

NATURE GENETICS
Volume 54, Issue 8, Pages 1227-+

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41588-022-01129-5

Keywords

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Funding

  1. DZHK [81Z0100103, 81Z0100112]
  2. Helmholtz Association [ERC-RA-0047]
  3. European Research Council Starting Grant [ERC-StG 715361 SPACEVAR]
  4. Fondation Leducq Transatlantic Networks Grant [16CVD03]
  5. Helmholtz Incubator grant [Sparse2Big ZT-I-0007]
  6. Studienstiftung des deutschen Volkes
  7. Max Planck Society
  8. DFG SFB 1366/project A4 [394046768]
  9. Leducq Foundation
  10. Boehringer Ingelheim Fonds PhD fellowship

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This study identifies specialized activated fibroblast cell states in the regenerating zebrafish heart using single-cell transcriptomics and spatiotemporal analysis, and reveals the origin of these cell states and the regulatory mechanism of endocardial fibroblast response.
Single-cell RNA sequencing and spatiotemporal analysis of the regenerating zebrafish heart identify transient proregenerative fibroblast-like cells that are derived from the epicardium and the endocardium. Wnt signalling regulates the endocardial fibroblast response. The adult zebrafish heart has a high capacity for regeneration following injury. However, the composition of the regenerative niche has remained largely elusive. Here, we dissected the diversity of activated cell states in the regenerating zebrafish heart based on single-cell transcriptomics and spatiotemporal analysis. We observed the emergence of several transient cell states with fibroblast characteristics following injury, and we outlined the proregenerative function of collagen-12-expressing fibroblasts. To understand the cascade of events leading to heart regeneration, we determined the origin of these cell states by high-throughput lineage tracing. We found that activated fibroblasts were derived from two separate sources: the epicardium and the endocardium. Mechanistically, we determined Wnt signalling as a regulator of the endocardial fibroblast response. In summary, our work identifies specialized activated fibroblast cell states that contribute to heart regeneration, thereby opening up possible approaches to modulating the regenerative capacity of the vertebrate heart.

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