Nityakalyani Srinivas, Peter Jetter, Bernhard J Ueberbacher, Martina Werneburg, Katja Zerbe, Jessica Steinmann, Benjamin Van der Meijden, Francesca Bernardini, Alexander Lederer, Ricardo L A Dias, Pauline E Misson, Heiko Henze, Jürg Zumbrunn, Frank O Gombert, Daniel Obrecht, Peter Hunziker, Stefan Schauer, Urs Ziegler, Andres Käch, Leo Eberl, Kathrin Riedel, Steven J DeMarco, John A Robinson
Index: Science 327(5968) , 1010-1013, (2010)
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Antibiotics with new mechanisms of action are urgently required to combat the growing health threat posed by resistant pathogenic microorganisms. We synthesized a family of peptidomimetic antibiotics based on the antimicrobial peptide protegrin I. Several rounds of optimization gave a lead compound that was active in the nanomolar range against Gram-negative Pseudomonas spp., but was largely inactive against other Gram-negative and Gram-positive bacteria. Biochemical and genetic studies showed that the peptidomimetics had a non-membrane-lytic mechanism of action and identified a homolog of the beta-barrel protein LptD (Imp/OstA), which functions in outer-membrane biogenesis, as a cellular target. The peptidomimetic showed potent antimicrobial activity in a mouse septicemia infection model. Drug-resistant strains of Pseudomonas are a serious health problem, so this family of antibiotics may have important therapeutic applications.
Structure | Name/CAS No. | Molecular Formula | Articles |
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ASB-14
CAS:216667-08-2 |
C22H46N2O4S |
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2007-06-01 [Mol. Cancer Ther. 6 , 1898-1908, (2007)] |
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2013-05-01 [Acta Biomater. 9(5) , 6492-501, (2013)] |
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