Synthesis, Receptor Binding, Molecular Modeling, and Proliferative Assays of a Series of 17α-Arylestradiols

A series of new derivatives of estradiol substituted at position 17α by various aryls has been synthesized. This was made possible by efficient activation methods for the addition of aryllithiums to the carbonyl group at position 17 of estrone by using tetramethylethylenediamine (TMEDA) or BF₃⋅OEt₂....

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Published in:Chembiochem : a European journal of chemical biology 2003-06, Vol.4 (6), p.494-503
Main Authors: Foy, Nicolas, Stéphan, Elie, Vessières, Anne, Salomon, Emmanuel, Heldt, Jan-Martin, Huché, Michel, Jaouen, Gérard
Format: Article
Language:English
Subjects:
arylation
estradiol
receptors
steroids
triazenes
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Summary:A series of new derivatives of estradiol substituted at position 17α by various aryls has been synthesized. This was made possible by efficient activation methods for the addition of aryllithiums to the carbonyl group at position 17 of estrone by using tetramethylethylenediamine (TMEDA) or BF₃⋅OEt₂. Their relative binding affinity (RBA) for the α and the β forms of the estrogen receptor (ER) have been measured. All except one of the compounds synthesized had an RBA value of around 10 % which indicates a level of tolerance towards the bulky substituent at position 17. The lipophilicity values measured for these compounds are higher than that found for estradiol (E₂). A study of their proliferative/antiproliferative effects was carried out on hormone-dependent (MCF7) and hormone-independent (MDA-MB231) breast cancer cell lines. It is interesting to note that all the compounds are estrogenic. The possibility of easily attaching an iodine at the end of a phenyl spacer opens up a route to new radiopharmaceuticals for use in radioimaging.
ISSN:1439-4227
1439-7633
DOI:10.1002/cbic.200200499