Structural Basis for the Inhibition of Cyclin G-Associated Kinase by Gefitinib.
Naomi OhbayashiKazutaka MurayamaMiyuki Kato-MurayamaMutsuko Kukimoto-NiinoTamami UejimaTakayoshi MatsudaNoboru OhsawaShigeyuki YokoyomaHiroshi NojimaMikako ShirouzuPublished in: ChemistryOpen (2018)
Gefitinib is the molecular target drug for advanced non-small-cell lung cancer. The primary target of gefitinib is the positive mutation of epidermal growth factor receptor, but it also inhibits cyclin G-associated kinase (GAK). To reveal the molecular bases of GAK and gefitinib binding, structure analyses were conducted and determined two forms of the gefitinib-bound nanobody⋅GAK kinase domain complex structures. The first form, GAK_1, has one gefitinib at the ATP binding pocket, whereas the second form, GAK_2, binds one each in the ATP binding site and a novel binding site adjacent to the activation segment C-terminal helix, a unique element of the Numb-associated kinase family. In the novel binding site, gefitinib binds in the hydrophobic groove around the activation segment, disrupting the conserved hydrogen bonds for the catalytic activity. These structures suggest possibilities for the development of selective GAK inhibitors for viral infections, such as the hepatitis C virus.
Keyphrases
- epidermal growth factor receptor
- tyrosine kinase
- advanced non small cell lung cancer
- small cell lung cancer
- hepatitis c virus
- protein kinase
- structural basis
- high resolution
- dna binding
- human immunodeficiency virus
- cell cycle
- genome wide
- emergency department
- gene expression
- mass spectrometry
- single cell
- pi k akt
- hiv infected