Abstract
Hsp90 shows great promise as a therapeutic target due to its potential to disable multiple signaling pathways simultaneously. In this study, we discovered that a natural product, butein moderately inhibited the growth of drug-resistant cancer cells (A2780cis and H1975), and brought about the degradation of oncogenic Hsp90 client proteins. The study demonstrated that butein would be a therapeutic lead to circumvent drug-resistance in cancer chemotherapy. The structure-based screening, synthesis, and biological evaluation of butein are described herein.
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Seo, Y. H. (2013). Butein disrupts hsp90’s molecular chaperoning function and exhibits anti-proliferative effects against drug-resistant cancer cells. Bulletin of the Korean Chemical Society, 34(11), 3345–3349. https://doi.org/10.5012/bkcs.2013.34.11.3345
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