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Exploring the mode-of-action of bioactive compounds by chemical-genetic profiling in yeast
Authors:Parsons Ainslie B  Lopez Andres  Givoni Inmar E  Williams David E  Gray Christopher A  Porter Justin  Chua Gordon  Sopko Richelle  Brost Renee L  Ho Cheuk-Hei  Wang Jiyi  Ketela Troy  Brenner Charles  Brill Julie A  Fernandez G Esteban  Lorenz Todd C  Payne Gregory S  Ishihara Satoru  Ohya Yoshikazu  Andrews Brenda  Hughes Timothy R  Frey Brendan J  Graham Todd R  Andersen Raymond J  Boone Charles
Institution:Banting and Best Department of Medical Research, University of Toronto, Toronto, Ontario M5G 1L6, Canada.
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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