Novel substrate prediction for the TAM family of RTKs using phosphoproteomics and structure-based modeling

Abstract: The TAM family of receptor tyrosine kinases is implicated in multiple distinct oncogenic signaling pathways. However, to date there are no FDA-approved small molecule inhibitors for the TAM kinases. Inhibitor design and screening rely on tools to study kinase activity. Our goal was to address this gap by designing a set of synthetic peptide substrates for each of the TAM family members: Tyro3, Axl and Mer. We used an in vitro phosphoproteomics workflow to determine the substrate profile of each TAM kinase and … Show more