Establishing selectivity of FAK-paxillin PPI inhibitor using pulldown proteomics and a focal adhesion protein selectivity panel
Hunter O'Brien, Brock Hay, Huzaifah Sheikh, Liam McCreary, Krishna Parsawar, Timothy Marlowe

TL;DR
Researchers developed a method to test how selective a drug is at inhibiting a specific protein interaction in melanoma cells.
Contribution
A novel pulldown-MS approach and focal adhesion protein selectivity panel were developed to assess PPI inhibitor selectivity.
Findings
UA-1907 binds with nanomolar affinity to the FAK FAT domain.
Other focal adhesion proteins showed no binding to UA-1907.
The pulldown-MS method successfully identified specific drug interactors.
Abstract
UA-2012 (and related non-myristoylated analog UA-1907) is a lead alpha-helical cyclic peptide which inhibits the focal adhesion kinase (FAK)-paxillin protein-protein interaction (PPI) and is being evaluated for the treatment of cutaneous melanoma. However, the development of an empirical approach to measure PPI inhibitor selectivity remains an important need. We report the development of a pulldown-MS proteomic approach, including a custom synthesized non-myristoylated UA-1907-agarose probe, to evaluate the binding selectivity of candidate FAK PPI inhibitors. Melanoma lysates were probed with UA-1907-conjugated agarose beads and eluted associated proteins were analyzed through untagged mass-spectroscopy proteomics. The identified proteins led to the development of a custom focal adhesion (FA) selectivity panel comprised of recombinant VinT, VinH, PARVA, PARVB, Talin-1 Rod 8, and the FAK…
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Taxonomy
TopicsCell Adhesion Molecules Research · Cellular Mechanics and Interactions · Cellular transport and secretion
