DNA site-specific N3-adenine methylation targeted to estrogen receptor-positive cells

A compound that can target cells expressing the estrogen receptor (ER), and produce predominantly 3-MeA adducts in those cells has been designed and synthesized. This compound produces mainly the 3-MeA adduct upon reaction with calf thymus DNA, and binds to the ER with a relative binding affinity of...

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Veröffentlicht in:Bioorganic & medicinal chemistry 2011-09, Vol.19 (17), p.5093-5102
Hauptverfasser: Kishton, Rigel J., Miller, Sean E., Perry, Heather, Lynch, Tera, Patel, Mayur, Gore, Vinayak K., Akkaraju, Giridhar R., Varadarajan, Sridhar
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Sprache:eng
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Zusammenfassung:A compound that can target cells expressing the estrogen receptor (ER), and produce predominantly 3-MeA adducts in those cells has been designed and synthesized. This compound produces mainly the 3-MeA adduct upon reaction with calf thymus DNA, and binds to the ER with a relative binding affinity of 51% (estradiol = 100%). The compound is toxic to ER-expressing MCF-7 breast cancer cells, and pre-treatment with the ER antagonist fulvestrant abrogates the toxicity. Pre-treatment of MCF-7 cells with netropsin, which inhibits N3-adenine methylation by the compound, resulted in a threefold decrease in the toxicity. These results demonstrate the feasibility of this strategy for producing 3-MeA adducts in targeted cells.
ISSN:0968-0896
1464-3391
DOI:10.1016/j.bmc.2011.07.026