Leveraging Peptide Substrate Libraries to Design Inhibitors of Bacterial Lon Protease

Overview

Journal ACS Chem Biol

Publisher American Chemical Society

Specialties Biochemistry
Biology

Date 2019 Aug 30

PMID 31464417

Citations 9

Authors

Brett M Babin

Paulina Kasperkiewicz

Tomasz Janiszewski

Euna Yoo

Marcin Dra G

Matthew Bogyo

Affiliations

Soon will be listed here.

Abstract

Lon is a widely conserved housekeeping protease found in all domains of life. Bacterial Lon is involved in recovery from various types of stress, including tolerance to fluoroquinolone antibiotics, and is linked to pathogenesis in a number of organisms. However, detailed functional studies of Lon have been limited by the lack of selective, cell-permeant inhibitors. Here, we describe the use of positional scanning libraries of hybrid peptide substrates to profile the primary sequence specificity of bacterial Lon. In addition to identifying optimal natural amino acid binding preferences, we identified several non-natural residues that were leveraged to develop optimal peptide substrates as well as a potent peptidic boronic acid inhibitor of Lon. Treatment of with this inhibitor promotes UV-induced filamentation and reduces tolerance to ciprofloxacin, phenocopying established -deletion phenotypes. It is also nontoxic to mammalian cells due to its selectivity for Lon over the proteasome. Our results provide new insight into the primary substrate specificity of Lon and identify substrates and an inhibitor that will serve as useful tools for dissecting the diverse cellular functions of Lon.

Citing Articles

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