Frontiers in Molecular Biosciences (May 2020)

Structure and Characterization of a Covalent Inhibitor of Src Kinase

  • Deepak Gurbani,
  • Guangyan Du,
  • Guangyan Du,
  • Nathaniel J. Henning,
  • Nathaniel J. Henning,
  • Suman Rao,
  • Suman Rao,
  • Suman Rao,
  • Asim K. Bera,
  • Tinghu Zhang,
  • Tinghu Zhang,
  • Nathanael S. Gray,
  • Nathanael S. Gray,
  • Kenneth D. Westover

DOI
https://doi.org/10.3389/fmolb.2020.00081
Journal volume & issue
Vol. 7

Abstract

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Unregulated Src activity promotes malignant processes in cancer, but no Src-directed targeted therapies are used clinically, possibly because early Src inhibitors produce off-target effects leading to toxicity. Improved selective Src inhibitors may enable Src-directed therapies. Previously, we reported an irreversible Src inhibitor, DGY-06-116, based on the hybridization of dasatinib and a promiscuous covalent kinase probe SM1-71. Here, we report biochemical and biophysical characterization of this compound. An x-ray co-crystal structure of DGY-06-116: Src shows a covalent interaction with the kinase p-loop and occupancy of the back hydrophobic kinase pocket, explaining its high potency, and selectivity. However, a reversible analog also shows similar potency. Kinetic analysis shows a slow inactivation rate compared to other clinically approved covalent kinase inhibitors, consistent with a need for p-loop movement prior to covalent bond formation. Overall, these results suggest that a strong reversible interaction is required to allow sufficient time for the covalent reaction to occur. Further optimization of the covalent linker may improve the kinetics of covalent bond formation.

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