4.8 Article

Synthesis of Biphenyl Proteomimetics as Estrogen Receptor-α Coactivator Binding Inhibitors

Journal

ORGANIC LETTERS
Volume 11, Issue 23, Pages 5370-5373

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/ol901999f

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Funding

  1. Department of Defense PCRP Concept [W81XWH04-1-0647]
  2. PCRP Training Award [W81XWH09-1-0208]
  3. National Institutes of Health [5R37 DK015556]
  4. NRSA [1 F30 ES016484-01, 5 T32 GM070421]

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A novel series of biphenyl proteomimetic compounds were designed as estrogen receptor-alpha (ER alpha) coactivator binding Inhibitors. Synthesis was accomplished through a convergent approach, employing Suzuki coupling chemistry to ligate the Individual modular units. Initial biological results support the ability of these compounds to compete for the ER alpha coactivator binding groove.

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