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Phenethyl pyridines with non-polar internal substitutents as selective ligands for estrogen receptor beta

机译:具有非极性内部取代酯的苯乙酰基吡啶作为雌激素受体β的选择性配体

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摘要

To create estrogen receptor beta (ERβ)-selective ligands with improved biological characteristics, we have extended our investigations of structurally simple bibenzyl-core ligands by preparing a series of compounds in which one phenol is replaced by a 3-hydroxy-pyridine ring. These phenethyl pyridines were obtained by picoline anion alkylation, and compounds with different patterns of alkyl substitution on the central two-carbon unit were prepared. Binding affinities for ERα and ERβ were determined, and ligands with promising affinities and selectivities for ERβ were further tested for their gene transcriptional activity. Several compounds had high affinity selectivity and good potency selectivity in transcription assays. This study advances our understanding of compounds having ER-subtype selectivity and will help to direct efforts in developing novel ER ligands.

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