De Novo Design of Boron-Based Peptidomimetics as Potent Inhibitors of Human ClpP in the Presence of Human ClpX.
Joanne TanJulie J GrouleffYulia JitkovaDiego B DiazElizabeth C GriffithWenjie ShaoAnastasia F BogdanchikovaGennady PodaAaron D SchimmerRichard E LeeAndrei K YudinPublished in: Journal of medicinal chemistry (2019)
Boronic acids have attracted the attention of synthetic and medicinal chemists due to boron's ability to modulate enzyme function. Recently, we demonstrated that boron-containing amphoteric building blocks facilitate the discovery of bioactive aminoboronic acids. Herein, we have augmented this capability with a de novo library design and a virtual screening platform modified for covalent ligands. This technique has allowed us to rapidly design and identify a series of α-aminoboronic acids as the first inhibitors of human ClpXP, which is responsible for the degradation of misfolded proteins.