A New Series of N5 Derivatives of the 1,1,5-Trimethyl Furo[3,4-c]pyridine-3,4-dione (Cerpegin) Selectively Inhibits the Post-Acid Activity of Mammalian 20S Proteasomes.

A large set of N5-derivatives of cerpegin (1,1,5-trimethyl furo[3,4-c]pyridine-3,4-dione) was designed and synthesized in high yields by a simple and handy method using various primary amines for a pyridine cycle synthesis. The effects of 29 derivatives on the three types of catalytic sites of purified mammalian 20S proteasomes (CT-L, T-L and PA) were measured. Most of the new compounds specifically inhibited the PA activity, in the micromolar range. Docking experiments support these results. Moreover, neither calpain I nor cathepsin B were inhibited.