AI Article Synopsis

  • Researchers screened over 500 fungal extracts from the Sonoran Desert to find small molecule inhibitors of Hsp90 using a two-stage testing approach that included a heat shock induction assay and a luciferase refolding assay.
  • The inhibitors radicicol and monocillin I were isolated from active extracts obtained from the fungi Chaetomium chiversii and Paraphaeosphaeria quadriseptata, respectively.
  • Subsequent studies evaluated the antiproliferative effects of these inhibitors on breast cancer cells and their ability to bind to Hsp90 and reduce levels of cancer-relevant proteins, suggesting these compounds could be promising for cancer treatment.

Article Abstract

In an effort to discover small molecule inhibitors of Hsp90, we have screened over 500 EtOAc extracts of Sonoran desert plant-associated fungi using a two-stage strategy consisting of a primary cell-based heat shock induction assay (HSIA) followed by a secondary biochemical luciferase refolding assay (LRA). Bioassay-guided fractionation of extracts active in these assays derived from Chaetomium chiversii and Paraphaeosphaeria quadriseptata furnished the Hsp90 inhibitors radicicol (1) and monocillin I (2), respectively. In SAR studies, 1, 2, and their analogues, 3-16, were evaluated in these assays, and the antiproliferative activity of compounds active in both assays was determined using the breast cancer cell line MCF-7. Radicicol and monocillin I were also evaluated in a solid-phase competition assay for their ability to bind Hsp90 and to deplete cellular levels of two known Hsp90 client proteins with relevance to breast cancer, estrogen receptor (ER), and the type 1 insulin-like growth factor receptor (IGF-1R). Some inferences on SAR were made considering the crystal structure of the N-terminus of yeast Hsp90 bound to 1 and the observed biological activities of 1-16. Isolation of radicicol and monocillin I in this study provides evidence that we have developed an effective strategy for discovering natural product-based Hsp90 inhibitors with potential anticancer activity.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1876775PMC
http://dx.doi.org/10.1021/np058095bDOI Listing

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