Novel nonsteroidal selective estrogen receptor modulators. Carbon and heteroatom replacement of oxygen in the ethoxypiperidine region of raloxifene

…, JP Sluka, KM Duke, AW Glasebrook

文献索引：Schmid, Christopher R.; Sluka, James P.; Duke, Kristen M.; Glasebrook, Andrew W. Bioorganic and Medicinal Chemistry Letters, 1999 , vol. 9, # 4 p. 523 - 528

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被引用次数: 14

摘要

Compounds were synthesized where oxygen in the ethoxypiperidine region of raloxifene is replaced with carbon, sulfur, or nitrogen linkages. Thia-and aza-substituted compounds were prepared by novel methodology. The compounds were evaluated in vitro as selective estrogen receptor modulators (SERMs). Calculations suggested the compounds exhibit an ER-α binding affinity/conformational energy relationship.

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Protein structure-based design, synthesis, and biological ev...

[Varney, Michael D.; Palmer, Cindy L.; Romines III, William H.; Boritzki, Theodore; Margosiak, Stephen A.; Almassy, Robert; Janson, Cheryl A.; Bartlett, Charlotte; Howland, Eleanor J.; Ferre, Rosanne Journal of Medicinal Chemistry, 1997 , vol. 40, # 16 p. 2502 - 2524]

Discovery of highly selective EP4 receptor agonists that sti...

[Bioorganic and Medicinal Chemistry Letters, , vol. 16, # 7 p. 1799 - 1802]

Protein structure-based design, synthesis, and biological ev...

[Journal of Medicinal Chemistry, , vol. 40, # 16 p. 2502 - 2524]

Novel nonsteroidal selective estrogen receptor modulators. C...

[Bioorganic and Medicinal Chemistry Letters, , vol. 9, # 4 p. 523 - 528]

Discovery of highly selective EP4 receptor agonists that sti...

[Bioorganic and Medicinal Chemistry Letters, , vol. 16, # 7 p. 1799 - 1802]