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Synthetic studies of cystobactamids as antibiotics and bacterial imaging carriers lead to compounds with high efficacy. | LitMetric

There is an alarming scarcity of novel chemical matter with bioactivity against multidrug-resistant Gram-negative bacterial pathogens. Cystobactamids, recently discovered natural products from myxobacteria, are an exception to this trend. Their unusual chemical structure, composed of oligomeric -aminobenzoic acid moieties, is associated with a high antibiotic activity through the inhibition of gyrase. In this study, structural determinants of cystobactamid's antibacterial potency were defined at five positions, which were varied using three different synthetic routes to the cystobactamid scaffold. The potency against could be increased ten-fold to an MIC (minimum inhibitory concentration) of 0.06 μg mL, and the previously identified spectrum gap of could be closed compared to the natural products (MIC of 0.5 μg mL). Proteolytic degradation of cystobactamids by the resistance factor AlbD was prevented by an amide-triazole replacement. Conjugation of cystobactamid's N-terminal tetrapeptide to a Bodipy moiety induced the selective localization of the fluorophore for bacterial imaging purposes. Finally, a first proof of concept was obtained in an infection mouse model, where derivative led to the reduction of bacterial loads (cfu, colony-forming units) in muscle, lung and kidneys by five orders of magnitude compared to vehicle-treated mice. These findings qualify cystobactamids as highly promising lead structures against infections caused by Gram-positive and Gram-negative bacterial pathogens.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8148378PMC
http://dx.doi.org/10.1039/c9sc04769gDOI Listing

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