1. Targeting Ras-, Rho-, and Rab-family GTPases via a conserved cryptic pocket.
- Author
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Morstein, Johannes, Bowcut, Victoria, Fernando, Micah, Yang, Yue, Zhu, Lawrence, Jenkins, Meredith L., Evans, John T., Guiley, Keelan Z., Peacock, D. Matthew, Krahnke, Sophie, Lin, Zhi, Taran, Katrine A., Huang, Benjamin J., Stephen, Andrew G., Burke, John E., Lightstone, Felice C., and Shokat, Kevan M.
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GTPASE-activating protein , *GUANOSINE triphosphate , *SMALL molecules , *RHO GTPases , *RAS proteins - Abstract
The family of Ras-like GTPases consists of over 150 different members, regulated by an even larger number of guanine exchange factors (GEFs) and GTPase-activating proteins (GAPs) that comprise cellular switch networks that govern cell motility, growth, polarity, protein trafficking, and gene expression. Efforts to develop selective small molecule probes and drugs for these proteins have been hampered by the high affinity of guanosine triphosphate (GTP) and lack of allosteric regulatory sites. This paradigm was recently challenged by the discovery of a cryptic allosteric pocket in the switch II region of K-Ras. Here, we ask whether similar pockets are present in GTPases beyond K-Ras. We systematically surveyed members of the Ras, Rho, and Rab family of GTPases and found that many GTPases exhibit targetable switch II pockets. Notable differences in the composition and conservation of key residues offer potential for the development of optimized inhibitors for many members of this previously undruggable family. [Display omitted] • Druggable switch II pocket is present in many GTPases beyond K-Ras • Ligand-bound H-Ras, RalA, and Rab1A were characterized by X-ray or HDX-MS • Inhibition of GTPase function is demonstrated in vitro and in cells • Switch II pocket inhibitor analogs show improved labeling of Rho and Rab GTPases Morstein et al. demonstrate the feasibility of inhibiting GTPases beyond K-Ras, including various Ras-, Rho-, and Rab-family GTPases that were previously considered undruggable. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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