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Chlorotrianisene

Catalog No. DB00269 Name DrugBank
CAS Number 569-57-3 Website http://www.ualberta.ca/
M. F. C23H21ClO3 Telephone (780) 492-3111
M. W. 380.86404 Fax (780) 492-1071
Purity Email david.wishart@ualberta.ca
Storage Chembase ID: 154

SYNONYMS

IUPAC name
1-[2-chloro-1,2-bis(4-methoxyphenyl)ethenyl]-4-methoxybenzene
IUPAC Traditional name
1-[2-chloro-1,2-bis(4-methoxyphenyl)ethenyl]-4-methoxybenzene
Brand Name
Merbentul
Trianisestrol
Anisene
Clorestrolo
Clorotrisin
Hormonisene
Khlortrianizen
Rianil
Chlorotrisin
Metace
Tace
Tace-Fn
Synonyms
Chlorotrianisenum [INN-Latin]
Chlorotrianisine
Chlortrianisoestrolum
Clorotrianiseno [INN-Spanish]
Chlortrianisen
Chlortrianisenum
CTA
Chlortrianizen
Chlorotrianizen
Chlortrianisene
Chlortrianisestrol
Chloortrianisestrol
Chlorestrolo

DATABASE IDS

PubChem SID 46508811
CAS Number 569-57-3
PubChem CID 11289

PROPERTIES

Hydrophobicity(logP) 6.4

DETAILS

Description (English)
Item Information
Drug Groups approved
Description A powerful synthetic, non-steroidal estrogen. [PubChem]
Indication Used to treat symptoms of menopause, deficiencies in ovary function (including underdevelopment of female sexual characteristics and some types of infertility), and in rare cases, prostate cancer. Chlorotrianisene may also be used to prevent breast engorgement following childbirth.
Pharmacology Chlorotrianisene is a nonsteroidal synthetic estrogen. After menopause, when the body no longer produces estrogen, chlorotrianisene is used as a simple replacement of estrogen. The estrogen-stimulated endometrium may bleed within 48-72 hours after discontinuance of estrogen therapy. Paradoxically, prolonged estrogen therapy may cause shrinkage of the endometrium and an increase in size of the myometrium. Estrogens have a weak anabolic effect and may cause sodium retention with associated fluid retention and edema. Estrogens may also decrease elevated blood cholesterol and phospholipid concentrations. Estrogens affect bone by increasing calcium deposition and accelerating epiphyseal closure, following initial growth stimulation. During the preovulatory or nonovulatory phase of the menstrual cycle, estrogen is the principal determinant in the onset of menstruation. A decline of estrogenic activity at the end of the menstrual cycle also may induce menstruation; however, the cessation of progesterone secretion is the most important factor during the mature ovulatory phase of the menstrual cycle. The benefit derived from estrogen therapy in the prevention of postpartum breast engorgement must be carefully weighed against the potential increased risk of puerperal thromboembolism associated with the use of large doses of estrogens.
Toxicity Acute overdosage of large doses of oral contraceptives in chidren reportedly produces almost no toxicity except nausea and vomiting. Acute overdosage of estrogens may cause nausea, and withdrawal bleeding may occur in females.
Affected Organisms
Humans and other mammals
Biotransformation Metabolized principally in the liver, although the kidneys, gonads, and muscle tissues may be involved to some extent. The metabolic fate of the synthetic estrogens has not been fully elucidated.
Absorption Absorption following oral administration is rapid.
Protein Binding 50-80%
External Links
Wikipedia
Drugs.com

REFERENCES