posted on 2013-01-10, 00:00authored byStefan Fischer, Heike
K. Wentsch, Svenja C. Mayer-Wrangowski, Markus Zimmermann, Silke M. Bauer, Kirsten Storch, Raimund Niess, Solveigh C. Koeberle, Christian Grütter, Frank M. Boeckler, Daniel Rauh, Stefan A. Laufer
p38α mitogen-activated protein (MAP) kinase is
a main target
in drug research concerning inflammatory diseases. Nevertheless, no
inhibitor of p38α MAP kinase has been introduced to the market.
This might be attributed to the fact that there is no inhibitor which
combines outstanding activity in biological systems and selectivity.
Herein an approach to the development of such inhibitors on the basis
of the highly selective molecular probe Skepinone-L is described.
Introduction of a “deep pocket” moiety addressing the
DFG motif led to an increased activity of the compounds. Hydrophilic
moieties, addressing the solvent-exposed area adjacent to hydrophilic
region II, conserved a high activity of the compounds in a whole blood
assay. Combined with their outstanding selectivity and low ATP competitiveness,
these inhibitors are very interesting candidates for use in biological
systems and in therapy.