Abstract
BackgroundZebrafish is a clinically-relevant model of heart regeneration. Unlike mammals, it has a remarkable heart repair capacity after injury, and promises novel translational applications. Amputation and cryoinjury models are key research tools for understanding injury response and regeneration in vivo. An understanding of the transcriptional responses following injury is needed to identify key players of heart tissue repair, as well as potential targets for boosting this property in humans.ResultsWe investigated amputation and cryoinjury in vivo models of heart damage in the zebrafish through unbiased, integrative analyses of independent molecular datasets. To detect genes with potential biological roles, we derived computational prediction models with microarray data from heart amputation experiments. We focused on a top-ranked set of genes highly activated in the early post-injury stage, whose activity was further verified in independent microarray datasets. Next, we performed independent validations of expression responses with qPCR in a cryoinjury model. Across in vivo models, the top candidates showed highly concordant responses at 1 and 3 days post-injury, which highlights the predictive power of our analysis strategies and the possible biological relevance of these genes. Top candidates are significantly involved in cell fate specification and differentiation, and include heart failure markers such as periostin, as well as potential new targets for heart regeneration. For example, ptgis and ca2 were overexpressed, while usp2a, a regulator of the p53 pathway, was down-regulated in our in vivo models. Interestingly, a high activity of ptgis and ca2 has been previously observed in failing hearts from rats and humans.ConclusionsWe identified genes with potential critical roles in the response to cardiac damage in the zebrafish. Their transcriptional activities are reproducible in different in vivo models of cardiac injury.Electronic supplementary materialThe online version of this article (doi:10.1186/1471-2164-15-852) contains supplementary material, which is available to authorized users.
Highlights
Zebrafish is a clinically-relevant model of heart regeneration
The zebrafish (Danio rerio) has the capacity to regenerate its heart after undergoing severe injury [1,2]
This capability has been shown in adult zebrafish using different in vivo models of cardiac damage, and involves the generation of new cardiomyocytes from existing ones located near the injury site [3,4]
Summary
Zebrafish is a clinically-relevant model of heart regeneration Unlike mammals, it has a remarkable heart repair capacity after injury, and promises novel translational applications. The zebrafish (Danio rerio) has the capacity to regenerate its heart after undergoing severe injury [1,2]. This capability has been shown in adult zebrafish using different in vivo models of cardiac damage, and involves the generation of new cardiomyocytes from existing ones located near the injury site [3,4]. The zebrafish represents a compelling model to study heart injury and regeneration with potential clinical impact. Response to drugs is well conserved between fish and mammals [18], making zebrafish a widely used model for toxicological analysis and to study the possible cardiac effects of chemical compounds
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