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      THE BINDING OF [3H]-OESTRADIOL-17β IN THE IMMATURE RAT UTERUS DURING THE SEQUENTIAL ADMINISTRATION OF NONSTEROIDAL ANTI-OESTROGENS

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      British Journal of Pharmacology
      Wiley

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          A monohydroxylated metabolite of tamoxifen with potent antioestrogenic activity.

          The oestrogenic and antioestrogenic properties of tamoxifen and its monohydroxylated (monohydroxytamoxifen) and dihydroxylated (dihydroxytamoxifen) metabolites have been investigated in the immature rat. Whether administered orally or subcutaneously, monohydroxytamoxifen was more active than tamoxifen as an antioestrogen. Dihydroxytamoxifen was less active than tamoxifen as an antioestrogen, but this derivative alone was unable to induce a uterotrophic response. Both metabolites of tamoxifen were potent inhibitors of the binding of [3H]oestradiol to oestrogen receptors in vitro. It is possible that the metabolites play a supportive role in the antioestrogenic activity of tamoxifen. The potent activity of monohydroxytamoxifen in vivo and in vitro suggests that this compound could be an important new tool for the subcellular investigation of oestrogenic and antioestrogenic events.
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            Estrogen-Receptor Interaction: Estrogenic hormones effect transformation of specific receptor proteins to a biochemically functional form

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              Effect of tamoxifen (ICI 46,474) on initiation and growth of DMBA-induced rat mammary carcinomata.

              V. Jordan (1976)
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                Author and article information

                Journal
                British Journal of Pharmacology
                Wiley
                00071188
                February 1979
                February 1979
                May 18 2015
                : 65
                : 2
                : 167-173
                Article
                10.1111/j.1476-5381.1979.tb07815.x
                b322fd06-d41b-48bb-8113-b4ec915067ef
                © 2015

                http://doi.wiley.com/10.1002/tdm_license_1.1

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