Discovery of FabH/FabF Inhibitors from Natural Products

Author:

Young Katherine1,Jayasuriya Hiranthi1,Ondeyka John G.1,Herath Kithsiri1,Zhang Chaowei1,Kodali Srinivas1,Galgoci Andrew1,Painter Ronald1,Brown-Driver Vickie1,Yamamoto Robert1,Silver Lynn L.1,Zheng Yingcong1,Ventura Judith I.1,Sigmund Janet1,Ha Sookhee1,Basilio Angela1,Vicente Francisca1,Tormo José Rubén1,Pelaez Fernando1,Youngman Phil1,Cully Doris1,Barrett John F.1,Schmatz Dennis1,Singh Sheo B.1,Wang Jun1

Affiliation:

1. Merck Research Laboratories, Rahway, New Jersey 07065

Abstract

ABSTRACT Condensing enzymes are essential in type II fatty acid synthesis and are promising targets for antibacterial drug discovery. Recently, a new approach using a xylose-inducible plasmid to express antisense RNA in Staphylococcus aureus has been described; however, the actual mechanism was not delineated. In this paper, the mechanism of decreased target protein production by expression of antisense RNA was investigated using Northern blotting. This revealed that the antisense RNA acts posttranscriptionally by targeting mRNA, leading to 5′ mRNA degradation. Using this technology, a two-plate assay was developed in order to identify FabF/FabH target-specific cell-permeable inhibitors by screening of natural product extracts. Over 250,000 natural product fermentation broths were screened and then confirmed in biochemical assays, yielding a hit rate of 0.1%. All known natural product FabH and FabF inhibitors, including cerulenin, thiolactomycin, thiotetromycin, and Tü3010, were discovered using this whole-cell mechanism-based screening approach. Phomallenic acids, which are new inhibitors of FabF, were also discovered. These new inhibitors exhibited target selectivity in the gel elongation assay and in the whole-cell-based two-plate assay. Phomallenic acid C showed good antibacterial activity, about 20-fold better than that of thiolactomycin and cerulenin, against S. aureus . It exhibited a spectrum of antibacterial activity against clinically important pathogens including methicillin-resistant Staphylococcus aureus , Bacillus subtilis , and Haemophilus influenzae .

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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