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A High-Content Screen Reveals New Small-Molecule Enhancers of Ras/Mapk Signaling as Probes for Zebrafish Heart Development

Zebrafish is the preferred vertebrate model for high throughput chemical screens to discover modulators of complex biological pathways. We adapted a transgenic zebrafish line, Tg(dusp6:EGFP), which reports on fibroblast growth factor (Fgf)/Ras/Mapk activity, into a quantitative, high-content chemica...

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Autores principales: Saydmohammed, Manush, Vollmer, Laura L., Onuoha, Ezenwa O., Maskrey, Taber S., Gibson, Gregory, Watkins, Simon C., Wipf, Peter, Vogt, Andreas, Tsang, Michael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6099644/
https://www.ncbi.nlm.nih.gov/pubmed/29997348
http://dx.doi.org/10.3390/molecules23071691
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author Saydmohammed, Manush
Vollmer, Laura L.
Onuoha, Ezenwa O.
Maskrey, Taber S.
Gibson, Gregory
Watkins, Simon C.
Wipf, Peter
Vogt, Andreas
Tsang, Michael
author_facet Saydmohammed, Manush
Vollmer, Laura L.
Onuoha, Ezenwa O.
Maskrey, Taber S.
Gibson, Gregory
Watkins, Simon C.
Wipf, Peter
Vogt, Andreas
Tsang, Michael
author_sort Saydmohammed, Manush
collection PubMed
description Zebrafish is the preferred vertebrate model for high throughput chemical screens to discover modulators of complex biological pathways. We adapted a transgenic zebrafish line, Tg(dusp6:EGFP), which reports on fibroblast growth factor (Fgf)/Ras/Mapk activity, into a quantitative, high-content chemical screen to identify novel Fgf hyperactivators as chemical probes for zebrafish heart development and regeneration. We screened 10,000 compounds from the TimTec ActiProbe library, and identified several structurally distinct classes of molecules that enhanced Fgf/Ras/Mapk signaling. We chose three agents—ST020101, ST011282, and ST006994—for confirmatory and functional studies based on potency, repeatability with repurchased material, favorable whole organism toxicity, and evidence of structure–activity relationships. Functional follow-up assays confirmed that all three compounds induced the expression of Fgf target genes during zebrafish embryonic development. Moreover, these compounds increased cardiac progenitor populations by effecting a fate change from endothelial to cardiac progenitors that translated into increased numbers of cardiomyocytes. Interestingly, ST006994 augmented Fgf/Ras/Mapk signaling without increasing Erk phosphorylation, suggesting a molecular mechanism of action downstream of Erk. We posit that the ST006994 pharmacophore could become a unique chemical probe to uncover novel mechanisms of Fgf signaling during heart development and regeneration downstream of the Mapk signaling node.
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spelling pubmed-60996442018-11-13 A High-Content Screen Reveals New Small-Molecule Enhancers of Ras/Mapk Signaling as Probes for Zebrafish Heart Development Saydmohammed, Manush Vollmer, Laura L. Onuoha, Ezenwa O. Maskrey, Taber S. Gibson, Gregory Watkins, Simon C. Wipf, Peter Vogt, Andreas Tsang, Michael Molecules Article Zebrafish is the preferred vertebrate model for high throughput chemical screens to discover modulators of complex biological pathways. We adapted a transgenic zebrafish line, Tg(dusp6:EGFP), which reports on fibroblast growth factor (Fgf)/Ras/Mapk activity, into a quantitative, high-content chemical screen to identify novel Fgf hyperactivators as chemical probes for zebrafish heart development and regeneration. We screened 10,000 compounds from the TimTec ActiProbe library, and identified several structurally distinct classes of molecules that enhanced Fgf/Ras/Mapk signaling. We chose three agents—ST020101, ST011282, and ST006994—for confirmatory and functional studies based on potency, repeatability with repurchased material, favorable whole organism toxicity, and evidence of structure–activity relationships. Functional follow-up assays confirmed that all three compounds induced the expression of Fgf target genes during zebrafish embryonic development. Moreover, these compounds increased cardiac progenitor populations by effecting a fate change from endothelial to cardiac progenitors that translated into increased numbers of cardiomyocytes. Interestingly, ST006994 augmented Fgf/Ras/Mapk signaling without increasing Erk phosphorylation, suggesting a molecular mechanism of action downstream of Erk. We posit that the ST006994 pharmacophore could become a unique chemical probe to uncover novel mechanisms of Fgf signaling during heart development and regeneration downstream of the Mapk signaling node. MDPI 2018-07-11 /pmc/articles/PMC6099644/ /pubmed/29997348 http://dx.doi.org/10.3390/molecules23071691 Text en © 2018 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Saydmohammed, Manush
Vollmer, Laura L.
Onuoha, Ezenwa O.
Maskrey, Taber S.
Gibson, Gregory
Watkins, Simon C.
Wipf, Peter
Vogt, Andreas
Tsang, Michael
A High-Content Screen Reveals New Small-Molecule Enhancers of Ras/Mapk Signaling as Probes for Zebrafish Heart Development
title A High-Content Screen Reveals New Small-Molecule Enhancers of Ras/Mapk Signaling as Probes for Zebrafish Heart Development
title_full A High-Content Screen Reveals New Small-Molecule Enhancers of Ras/Mapk Signaling as Probes for Zebrafish Heart Development
title_fullStr A High-Content Screen Reveals New Small-Molecule Enhancers of Ras/Mapk Signaling as Probes for Zebrafish Heart Development
title_full_unstemmed A High-Content Screen Reveals New Small-Molecule Enhancers of Ras/Mapk Signaling as Probes for Zebrafish Heart Development
title_short A High-Content Screen Reveals New Small-Molecule Enhancers of Ras/Mapk Signaling as Probes for Zebrafish Heart Development
title_sort high-content screen reveals new small-molecule enhancers of ras/mapk signaling as probes for zebrafish heart development
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6099644/
https://www.ncbi.nlm.nih.gov/pubmed/29997348
http://dx.doi.org/10.3390/molecules23071691
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