4.7 Article

Triaryl-Substituted Schiff Bases Are High-Affinity Subtype-Selective Ligands for the Estrogen Receptor

Journal

JOURNAL OF MEDICINAL CHEMISTRY
Volume 57, Issue 8, Pages 3532-3545

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/jm500268j

Keywords

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Funding

  1. NSFC [91017005, 81172935, 81373255]
  2. Ministry of Education [313040]
  3. Scientific and Technological Innovative Research Team of Wuhan [2013070204020048]
  4. Hubei Province's Outstanding Medical Academic Leader Program
  5. Fundamental Research Funds for the Central Universities [201130602020001]
  6. National Institutes of Health [PHS 5R37 DK015556, 5R01 DK077085]
  7. Frenchman's Creek Women for Cancer Research

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We have explored the isoelectronic replacement of the C=C double bond found at the core of many nonsteroidal estrogen ligands with a simple Schiff base (C=N). Di- and triaryl-substituted imine derivatives were conveniently prepared by the condensation of benzophenones with various anilines without the need for phenolic hydroxy protection. Most of these imines demonstrated high affinity for the estrogen receptors, which, in some cases exceeded that of estradiol. In cell-based assays, these imines profiled as ER alpha agonists but as ER beta antagonists, showing preferential reliance on the N-terminal activation function (AF1), which is more active in ER alpha. X-ray analysis revealed that the triaryl-imines distort the ligand-binding pocket in a new way: by controlling the separation of helices 3 and 11, which appears to alter the C-terminal AF2 surface that binds transcriptional coactivators. This work suggests that C=N for C=C substitution might be more widely considered as a general strategy for preparing drug analogues.

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