Molecules (Oct 2014)

Structural Elucidation of the DFG-Asp in and DFG-Asp out States of TAM Kinases and Insight into the Selectivity of Their Inhibitors

  • Abdellah Messoussi,
  • Lucile Peyronnet,
  • Clémence Feneyrolles,
  • Gwénaël Chevé,
  • Khalid Bougrin,
  • Aziz Yasri

DOI
https://doi.org/10.3390/molecules191016223
Journal volume & issue
Vol. 19, no. 10
pp. 16223 – 16239

Abstract

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Structural elucidation of the active (DFG-Asp in) and inactive (DFG-Asp out) states of the TAM family of receptor tyrosine kinases is required for future development of TAM inhibitors as drugs. Herein we report a computational study on each of the three TAM members Tyro-3, Axl and Mer. DFG-Asp in and DFG-Asp out homology models of each one were built based on the X-ray structure of c-Met kinase, an enzyme with a closely related sequence. Structural validation and in silico screening enabled identification of critical amino acids for ligand binding within the active site of each DFG-Asp in and DFG-Asp out model. The position and nature of amino acids that differ among Tyro-3, Axl and Mer, and the potential role of these residues in the design of selective TAM ligands, are discussed.

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