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Structure-guided development of efficacious antifungal agents targeting Candida glabrata dihydrofolate reductase.


ABSTRACT: Candida glabrata is a lethal fungal pathogen resistant to many antifungal agents and has emerged as a critical target for drug discovery. Over the past several years, we have been developing a class of propargyl-linked antifolates as antimicrobials and hypothesized that these compounds could be effective inhibitors of dihydrofolate reductase (DHFR) from C. glabrata. We initially screened a small collection of these inhibitors and found modest levels of potency. Subsequently, we determined the crystal structure of C. glabrata DHFR bound to a representative inhibitor with data to 1.6 A resolution. Using this structure, we designed and synthesized second-generation inhibitors. These inhibitors bind the C. glabrata DHFR enzyme with subnanomolar potency, display greater than 2000-fold levels of selectivity over the human enzyme, and inhibit the growth of C. glabrata at levels observed with clinically employed therapeutics.

SUBMITTER: Liu J 

PROVIDER: S-EPMC2610858 | biostudies-literature | 2008 Sep

REPOSITORIES: biostudies-literature

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Structure-guided development of efficacious antifungal agents targeting Candida glabrata dihydrofolate reductase.

Liu Jieying J   Bolstad David B DB   Smith Adrienne E AE   Priestley Nigel D ND   Wright Dennis L DL   Anderson Amy C AC  

Chemistry & biology 20080901 9


Candida glabrata is a lethal fungal pathogen resistant to many antifungal agents and has emerged as a critical target for drug discovery. Over the past several years, we have been developing a class of propargyl-linked antifolates as antimicrobials and hypothesized that these compounds could be effective inhibitors of dihydrofolate reductase (DHFR) from C. glabrata. We initially screened a small collection of these inhibitors and found modest levels of potency. Subsequently, we determined the cr  ...[more]

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