Synthesis of Polyfluoro Ketones for Selective Inhibition of Human Phospholipase A2Enzymes

Abstract

The development of selective inhibitors for individual PLA₂ enzymes is necessary in order to target PLA₂-specific signaling pathways, but it is challenging due to the observed promiscuity of known PLA₂ inhibitors. In the current work, we present the development and application of a variety of synthetic routes to produce pentafluoro, tetrafluoro, and trifluoro derivatives of activated carbonyl groups in order to screen for selective inhibitors and characterize the chemical properties that can lead to selective inhibition. Our results demonstrate that the pentafluoroethyl ketone functionality favors selective inhibition of the GVIA iPLA₂, a very important enzyme for which specific, potent, reversible inhibitors are needed. We find that 1,1,1,2,2-pentafluoro-7-phenyl-heptan-3-one (FKGK11) is a selective inhibitor of GVIA iPLA₂ (X_I(50) = 0.0073). Furthermore, we conclude that the introduction of an additional fluorine atom at the α′ position of a trifluoromethyl ketone constitutes an important strategy for the development of new potent GVIA iPLA₂ inhibitors.