posted on 2015-01-08, 00:00authored byPaul Czodrowski, Günter Hölzemann, Gerhard Barnickel, Hartmut Greiner, Djordje Musil
In fragment-based screening, the
choice of the best suited fragment
hit among the detected hits is crucial for success. In our study,
a kinase lead compound was fragmented, the hinge-binding motif extracted
as a core fragment, and a minilibrary of five similar compounds with
fragment-like properties was selected from our proprietary compound
database. The structures of five fragments in complex with transforming
growth factor β receptor type 1 kinase domain were determined
by X-ray crystallography. Three different binding modes of the fragments
are observed that depend on the position and the type of the substitution
at the core fragment. The influence of different substituents on the
preferred fragment pose was analyzed by various computational approaches.
We postulate that the replacement of water molecules leads to the
different binding modes.