Journal
NATURE
Volume 464, Issue 7288, Pages 606-U168Publisher
NATURE PUBLISHING GROUP
DOI: 10.1038/nature08899
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Funding
- Ministry of Innovation, Universities and Enterprise (DIUE), Generalitat de Catalunya
- Fundacion Cellex
- Ipsen Foundation
- G. Harold and Leila Y. Mathers Charitable Foundation
- Sanofi-Aventis
- Ministry of Science and Innovation (MICINN)
- CIBER
- National Institutes of Health
- ICREA Funding Source: Custom
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Although mammalian hearts show almost no ability to regenerate, there is a growing initiative to determine whether existing cardiomyocytes or progenitor cells can be coaxed into eliciting a regenerative response. In contrast to mammals, several non-mammalian vertebrate species are able to regenerate their hearts(1-3), including the zebrafish(4,5), which can fully regenerate its heart after amputation of up to 20% of the ventricle. To address directly the source of newly formed cardiomyocytes during zebrafish heart regeneration, we first established a genetic strategy to trace the lineage of cardiomyocytes in the adult fish, on the basis of the Cre/lox system widely used in the mouse(6). Here we use this system to show that regenerated heart muscle cells are derived from the proliferation of differentiated cardiomyocytes. Furthermore, we show that proliferating cardiomyocytes undergo limited dedifferentiation characterized by the disassembly of their sarcomeric structure, detachment from one another and the expression of regulators of cell-cycle progression. Specifically, we show that the gene product of polo-like kinase 1 (plk1) is an essential component of cardiomyocyte proliferation during heart regeneration. Our data provide the first direct evidence for the source of proliferating cardiomyocytes during zebrafish heart regeneration and indicate that stem or progenitor cells are not significantly involved in this process.
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