Novel Small-Molecule Inhibitors of RNA Polymerase III
Author(s) -
Liping Wu,
Jing Pan,
Vala Thoroddsen,
Deborah R. Wysong,
Ronald K. Blackman,
Christine E. Bulawa,
Alexandra E. Gould,
Timothy D. Ocain,
Lawrence R. Dick,
Patrick R. Errada,
Patrick Dorr,
Tanya Parkinson,
Tony Wood,
Daniel Kornitzer,
Ziva Weissman,
Ian M. Willis,
Karen McGovern
Publication year - 2003
Publication title -
eukaryotic cell
Language(s) - English
Resource type - Journals
eISSN - 1535-9778
pISSN - 1535-9786
DOI - 10.1128/ec.2.2.256-264.2003
Subject(s) - rna polymerase iii , biology , rna polymerase ii , saccharomyces cerevisiae , transcription (linguistics) , rna , rna polymerase i , microbiology and biotechnology , transcription factor ii d , polymerase , rna polymerase , mutant , processivity , biochemistry , yeast , gene , gene expression , promoter , linguistics , philosophy
A genetic approach utilizing the yeast Saccharomyces cerevisiae was used to identify the target of antifungal compounds. This analysis led to the identification of small molecule inhibitors of RNA polymerase (Pol) III from Saccharomyces cerevisiae. Three lines of evidence show that UK-118005 inhibits cell growth by targeting RNA Pol III in yeast. First, a dominant mutation in the g domain of Rpo31p, the largest subunit of RNA Pol III, confers resistance to the compound. Second, UK-118005 rapidly inhibits tRNA synthesis in wild-type cells but not in UK-118005 resistant mutants. Third, in biochemical assays, UK-118005 inhibits tRNA gene transcription in vitro by the wild-type but not the mutant Pol III enzyme. By testing analogs of UK-118005 in a template-specific RNA Pol III transcription assay, an inhibitor with significantly higher potency, ML-60218, was identified. Further examination showed that both compounds are broad-spectrum inhibitors, displaying activity against RNA Pol III transcription systems derived from Candida albicans and human cells. The identification of these inhibitors demonstrates that RNA Pol III can be targeted by small synthetic molecules.
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