A substrate-free activity-based protein profiling screen for the discovery of selective PREPL inhibitors.

[cystinuria]

Peptidases play vital roles in physiology through the biosynthesis , degradation , and regulation of peptides . Prolyl endopeptidase-like (PREPL ) is a newly described member of the prolyl peptidase family , with significant homology to mammalian prolyl endopeptidase and the bacterial peptidase oligopeptidase B . The biochemistry and biology of PREPL are of fundamental interest due to this enzyme 's homology to the biomedically important prolyl peptidases and its localization in the central nervous system . Furthermore , genetic studies of patients suffering from hypotonia -cystinuria syndrome (HCS ) have revealed a deletion of a portion of the genome that includes the PREPL gene . HCS symptoms thought to be caused by lack of PREPL include neuromuscular and mild cognitive deficits . A number of complementary approaches , ranging from biochemistry to genetics , will be required to understand the biochemical , cellular , physiological , and pathological mechanisms regulated by PREPL . We are particularly interested in investigating physiological substrates and pathways controlled by PREPL . Here , we use a fluorescence polarization activity-based protein profiling (fluopol-ABPP ) assay to discover selective small -molecule inhibitors of PREPL . Fluopol-ABPP is a substrate-free approach that is ideally suited for studying serine hydrolases for which no substrates are known , such as PREPL . After screening over 300 ,000 compounds using fluopol-ABPP , we employed a number of secondary assays to confirm assay hits and characterize a group of 3 -oxo-1 -phenyl-2 ,3 ,5 ,6 ,7 ,8 -hexahydroisoquinoline-4 -carbonitrile and 1 -alkyl-3 -oxo-3 ,5 ,6 ,7 -tetrahydro-2 H -cyclopenta [c ]pyridine-4 -carbonitrile PREPL inhibitors that are able to block PREPL activity in cells . Moreover , when administered to mice , 1 -isobutyl-3 -oxo-3 ,5 ,6 ,7 -tetrahydro-2 H -cyclopenta [c ]pyridine-4 -carbonitrile distributes to the brain , indicating that it may be useful for in vivo studies . The application of fluopol-ABPP has led to the first reported PREPL inhibitors , and these inhibitors will be of great value in studying the biochemistry of PREPL and in eventually understanding the link between PREPL and HCS .