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Desmethyl Macrolides: Synthesis and Evaluation of 4,8-Didesmethyl Telithromycin.


ABSTRACT: There is an urgent need for novel sources of antibiotics to address the incessant and inevitable onset of bacterial resistance. To this end, we have initiated a structure-based drug design program that features a desmethylation strategy (i.e., replacing methyl groups with hydrogens). Herein we report the total synthesis, molecular modeling and biological evaluation of 4,8-didesmethyl telithromycin (5), a novel desmethyl analogue of the third-generation ketolide antibiotic telithromycin (2), which is an FDA-approved semisynthetic derivative of erythromycin (1). We found 4,8-didesmethyl telithromycin (5) to be eight times more active than previously prepared 4,8,10-tridesmethyl congener (3) and two times more active than 4,10-didesmethyl regioisomer (4) in MIC assays. While less potent than telithromycin (2) and paralleling the observations made in the previous study of 4,10-didesmethyl analogue (4), the inclusion of a single methyl group improves biological activity thus supporting its role in antibiotic activity.

SUBMITTER: Wagh B 

PROVIDER: S-EPMC3763958 | biostudies-literature | 2012 Dec

REPOSITORIES: biostudies-literature

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Desmethyl Macrolides: Synthesis and Evaluation of 4,8-Didesmethyl Telithromycin.

Wagh Bharat B   Paul Tapas T   Glassford Ian I   Debrosse Charles C   Klepacki Dorota D   Small Meagan C MC   Mackerell Alexander D AD   Andrade Rodrigo B RB  

ACS medicinal chemistry letters 20121201 12


There is an urgent need for novel sources of antibiotics to address the incessant and inevitable onset of bacterial resistance. To this end, we have initiated a structure-based drug design program that features a desmethylation strategy (i.e., replacing methyl groups with hydrogens). Herein we report the total synthesis, molecular modeling and biological evaluation of 4,8-didesmethyl telithromycin (<b>5</b>), a novel desmethyl analogue of the third-generation ketolide antibiotic telithromycin (<  ...[more]

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