1969
DOI: 10.1111/j.2042-7158.1969.tb08247.x
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Prolonged oestrogenic activity in rats after single oral administration of ethinyloestradiol-3-cyclopentyl ether

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Cited by 14 publications
(9 citation statements)
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“…The increase in lipophilicity due to an aromatic carbamate group could cause an accumulation of the prodrug in the fatty tissues of the organism after administration, with a resulting slow release into the blood circulation upon hydrolysis of the prodrug. This compartmental accumulation has also been described for other compounds including oestradiol derivatives (Giannina & Meli 1969;Gardi et a1 1973).…”
Section: Discussionsupporting
confidence: 59%
“…The increase in lipophilicity due to an aromatic carbamate group could cause an accumulation of the prodrug in the fatty tissues of the organism after administration, with a resulting slow release into the blood circulation upon hydrolysis of the prodrug. This compartmental accumulation has also been described for other compounds including oestradiol derivatives (Giannina & Meli 1969;Gardi et a1 1973).…”
Section: Discussionsupporting
confidence: 59%
“…This may be the case of bisether 30, which was found to be poorly active although the etherification at C-3 with cyclopentanol is known to endow most of the estrogens with a higher and long-lasting activity. [21][22][23] Like other lipophilic compounds,24 the labile estradiol 17-ethers are significantly absorbed and highly active after oral treatment mainly when given in oil solution. However, a too high lipophilicity may reduce the biological availability of the compound also after oral administration, as observed in the bisethers 6 and 70.…”
Section: Biology and Discussionmentioning
confidence: 99%
“…QUN is the 3-cyclopentyl ether of ethinyl estradiol (EE2), After oral administration, it is stored in adipose tissue where it is gradually released and metabolized principally to EE2 14 . The potent effect of QUN is approximately several times higher than EE2 with a very long biological half-life of more than 5 days 15 . The sulfate and glucuronate conjugates of QUN and EE2 are formed in the kidney and excreted by human and livestock in the urine, and they can be desulfated and deglucuronidated by corresponding enzymes in the environment and converted back into its precursors 16 .…”
Section: Introductionmentioning
confidence: 98%