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Identification of Kinases Activated by Multiple Pro-Angiogenic Growth Factors

Scott Gruver, Scott Rata, View ORCID ProfileLeonid Peshkin, View ORCID ProfileMarc W Kirschner
doi: https://doi.org/10.1101/2021.02.28.433132
Scott Gruver
1Department of Systems Biology, Harvard University Medical School; Boston, MA02115
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Scott Rata
1Department of Systems Biology, Harvard University Medical School; Boston, MA02115
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Leonid Peshkin
1Department of Systems Biology, Harvard University Medical School; Boston, MA02115
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  • For correspondence: marc@hms.harvard.edu pesha@hms.harvard.edu
Marc W Kirschner
1Department of Systems Biology, Harvard University Medical School; Boston, MA02115
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  • For correspondence: marc@hms.harvard.edu pesha@hms.harvard.edu
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ABSTRACT

Antiangiogenic therapy began as an effort to inhibit VEGF signaling, which was thought to be the sole factor driving tumor angiogenesis. It has become clear that there are more pro-angiogenic growth factors that can substitute for VEGF during tumor vascularization. This has led to the development of multi-kinase inhibitors which simultaneously target multiple growth factor receptors. These inhibitors perform better than monotherapies yet to date no multi-kinase inhibitor targets all receptors known to be involved in pro-angiogenic signaling and resistance inevitably occurs. Given the large number of pro-angiogenic growth factors identified, it may be impossible to simultaneously target all pro-angiogenic growth factor receptors. Here we search for kinase targets, some which may be intracellularly localized, that are critical in endothelial cell proliferation irrespective of the growth factor used. We develop a quantitative endothelial cell proliferation assay and combine it with “kinome regression” or KIR, a recently developed method capable of identifying kinases that influence a quantitative phenotype. We report the kinases implicated by KIR and provide orthogonal evidence of their importance in endothelial cell proliferation. Our approach may point to a new strategy to develop a more complete anti-angiogenic blockade.

Competing Interest Statement

The authors have declared no competing interest.

Footnotes

  • minor fixes in the text, mostly discussion and corrected Figure captions and labels

Copyright 
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY-NC-ND 4.0 International license.
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Posted November 14, 2022.
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Identification of Kinases Activated by Multiple Pro-Angiogenic Growth Factors
Scott Gruver, Scott Rata, Leonid Peshkin, Marc W Kirschner
bioRxiv 2021.02.28.433132; doi: https://doi.org/10.1101/2021.02.28.433132
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Identification of Kinases Activated by Multiple Pro-Angiogenic Growth Factors
Scott Gruver, Scott Rata, Leonid Peshkin, Marc W Kirschner
bioRxiv 2021.02.28.433132; doi: https://doi.org/10.1101/2021.02.28.433132

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