| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1391097 | Chemistry & Biology | 2014 | 10 Pages |
•Lassomycin has potent and selective bactericidal activity against M. tuberculosis•Lassomycin is a lasso peptide but lacks the family’s characteristic knot•Lassomycin activates ClpC1 ATP hydrolysis, uncoupling it from ClpP1P2 proteolysis
SummaryLanguishing antibiotic discovery and flourishing antibiotic resistance have prompted the development of alternative untapped sources for antibiotic discovery, including previously uncultured bacteria. Here, we screen extracts from uncultured species against Mycobacterium tuberculosis and identify lassomycin, an antibiotic that exhibits potent bactericidal activity against both growing and dormant mycobacteria, including drug-resistant forms of M. tuberculosis, but little activity against other bacteria or mammalian cells. Lassomycin is a highly basic, ribosomally encoded cyclic peptide with an unusual structural fold that only partially resembles that of other lasso peptides. We show that lassomycin binds to a highly acidic region of the ClpC1 ATPase complex and markedly stimulates its ATPase activity without stimulating ClpP1P2-catalyzed protein breakdown, which is essential for viability of mycobacteria. This mechanism, uncoupling ATPase from proteolytic activity, accounts for the bactericidal activity of lassomycin.
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