Synthesis of Homo A-CD Estrogens for Potential Use in Hormone Replacement Therapy
Hormone replacement therapy (HRT) has been subject to much debate due to concerns that long term use of such treatment of menopause increases the risk of breast and uterine cancer. This is thought to be caused by estradiol (1) binding to the estrogen receptor α (ERα) resulting in increased cell prol...
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Université d'Ottawa / University of Ottawa
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Online Access: | http://hdl.handle.net/10393/32082 http://dx.doi.org/10.20381/ruor-2783 |
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ndltd-uottawa.ca-oai-ruor.uottawa.ca-10393-320822018-01-05T19:02:14Z Synthesis of Homo A-CD Estrogens for Potential Use in Hormone Replacement Therapy Talbi, Oussama Durst, Tony Synthesis HRT Estrogen Hydride shift Hormone replacement therapy (HRT) has been subject to much debate due to concerns that long term use of such treatment of menopause increases the risk of breast and uterine cancer. This is thought to be caused by estradiol (1) binding to the estrogen receptor α (ERα) resulting in increased cell proliferation. Another possible mechanism relates to toxicity of the estrodiol metabolites, which are thought to be genotoxic ortho-quinones. In a previous project, a series of A-CD estrogens (2) were synthesised as non-carcinogenic estradiol agonists where the cis CD ring junction was thought to be the cause of the desirable selectivity for ERβ. In this thesis, homo A-CDs were synthesised (3) with expansion of the D ring thought to increase the selecitivty for ERβ. Relative Binding Affinities (RBA) were determined with selectivity to ERα and ERβ. Most ligands showed decreased selectivity when compared to the original A-CD series. However, compounds carrying the CF3 moiety continued to show very high potency. In addition, novel synthetic routes were employed in the preparation of certain compounds. 2015-02-17T12:54:20Z 2015-02-17T12:54:20Z 2015 2015 Thesis http://hdl.handle.net/10393/32082 http://dx.doi.org/10.20381/ruor-2783 en Université d'Ottawa / University of Ottawa |
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language |
en |
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topic |
Synthesis HRT Estrogen Hydride shift |
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Synthesis HRT Estrogen Hydride shift Talbi, Oussama Synthesis of Homo A-CD Estrogens for Potential Use in Hormone Replacement Therapy |
description |
Hormone replacement therapy (HRT) has been subject to much debate due to concerns that long term use of such treatment of menopause increases the risk of breast and uterine cancer. This is thought to be caused by estradiol (1) binding to the estrogen receptor α (ERα) resulting in increased cell proliferation. Another possible mechanism relates to toxicity of the estrodiol metabolites, which are thought to be genotoxic ortho-quinones. In a previous project, a series of A-CD estrogens (2) were synthesised as non-carcinogenic estradiol agonists where the cis CD ring junction was thought to be the cause of the desirable selectivity for ERβ. In this thesis, homo A-CDs were synthesised (3) with expansion of the D ring thought to increase the selecitivty for ERβ. Relative Binding Affinities (RBA) were determined with selectivity to ERα and ERβ. Most ligands showed decreased selectivity when compared to the original A-CD series. However, compounds carrying the CF3 moiety continued to show very high potency. In addition, novel synthetic routes were employed in the preparation of certain compounds. |
author2 |
Durst, Tony |
author_facet |
Durst, Tony Talbi, Oussama |
author |
Talbi, Oussama |
author_sort |
Talbi, Oussama |
title |
Synthesis of Homo A-CD Estrogens for Potential Use in Hormone Replacement Therapy |
title_short |
Synthesis of Homo A-CD Estrogens for Potential Use in Hormone Replacement Therapy |
title_full |
Synthesis of Homo A-CD Estrogens for Potential Use in Hormone Replacement Therapy |
title_fullStr |
Synthesis of Homo A-CD Estrogens for Potential Use in Hormone Replacement Therapy |
title_full_unstemmed |
Synthesis of Homo A-CD Estrogens for Potential Use in Hormone Replacement Therapy |
title_sort |
synthesis of homo a-cd estrogens for potential use in hormone replacement therapy |
publisher |
Université d'Ottawa / University of Ottawa |
publishDate |
2015 |
url |
http://hdl.handle.net/10393/32082 http://dx.doi.org/10.20381/ruor-2783 |
work_keys_str_mv |
AT talbioussama synthesisofhomoacdestrogensforpotentialuseinhormonereplacementtherapy |
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1718598236065759232 |