Toward Broad Spectrum DHFR inhibitors Targeting Trimethoprim Resistant Enzymes Identified in Clinical Isolates of Methicillin-Resistant Staphylococcus aureus

Author:

Reeve Stephanie M.ORCID,Si Debjani,Krucinska Jolanta,Yan Yongzhao,Viswanathan Kishore,Wang Siyu,Holt Graham T.,Frenkel Marcel S.,Ojewole Adegoke A.,Estrada Alexavier,Agabiti Sherry S.,Alverson Jeremy B.,Gibson Nathan D.,Priestly Nigel D.,Wiemer Andrew J.,Donald Bruce R.,Wright Dennis L.

Abstract

AbstractThe spread of plasmid borne resistance enzymes in clinical Staphylococcus aureus isolates is rendering trimethoprim and iclaprim, both inhibitors of dihydrofolate reductase (DHFR), ineffective. Continued exploitation of these targets will require compounds that can broadly inhibit these resistance-confering isoforms. Using a structure-based approach, we have developed a novel class of ionized non-classical antifolates (INCAs) that capture the molecular interactions that have been exclusive to classical antifolates. These modifications allow for a greatly expanded spectrum of activity across these pathogenic DHFR isoforms, while maintaining the ability to penetrate the bacterial cell wall. Using biochemical, structural and computational methods, we are able to optimize these inhibitors to the conserved active sites of the endogenous and trimethoprim resistant DHFR enzymes. Here, we report a series of INCA compounds that exhibit low nanomolar enzymatic activity and potent cellular activity with human selectivity against a panel of clinically relevant TMPR MRSA isolates.

Publisher

Cold Spring Harbor Laboratory

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