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      Exploring the mode-of-action of bioactive compounds by chemical-genetic profiling in yeast.

      Cell
      Antineoplastic Agents, Hormonal, pharmacology, Antiviral Agents, Cluster Analysis, Depsipeptides, Drug Evaluation, Preclinical, methods, Drug Resistance, genetics, Fungal Proteins, drug effects, metabolism, Gene Expression Profiling, Molecular Structure, Mutation, Pharmaceutical Preparations, chemistry, classification, Phosphatidylserines, Signal Transduction, Tamoxifen, Yeasts

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          Abstract

          Discovering target and off-target effects of specific compounds is critical to drug discovery and development. We generated a compendium of "chemical-genetic interaction" profiles by testing the collection of viable yeast haploid deletion mutants for hypersensitivity to 82 compounds and natural product extracts. To cluster compounds with a similar mode-of-action and to reveal insights into the cellular pathways and proteins affected, we applied both a hierarchical clustering and a factorgram method, which allows a gene or compound to be associated with more than one group. In particular, tamoxifen, a breast cancer therapeutic, was found to disrupt calcium homeostasis and phosphatidylserine (PS) was recognized as a target for papuamide B, a cytotoxic lipopeptide with anti-HIV activity. Further, the profile of crude extracts resembled that of its constituent purified natural product, enabling detailed classification of extract activity prior to purification. This compendium should serve as a valuable key for interpreting cellular effects of novel compounds with similar activities.

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