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Estradiol undecylate

August 27, 2023

Estradiol undecylate (EU or E2U), also known as estradiol undecanoate and formerly sold under the brand names Delestrec and Progynon Depot 100 among others, is an estrogen medication which has been used in the treatment of prostate cancer in men.[9][10][11][12][1] It has also been used as a part of hormone therapy for transgender women.[13][14][15] Although estradiol undecylate has been used in the past, it was discontinued and hence is no longer available.[11][16] The medication has been given by injection into muscle usually once a month.[1][17][12]

Estradiol undecylate
Clinical data
Pronunciation/ˌɛstrəˈdɒl ənˈdɛsɪlt/
ES-trə-DY-ol un-DESS-il-ayt
Trade namesDelestrec, Progynon Depot 100, others
Other namesEU; E2U; Estradiol undecanoate; Estradiol unducelate; RS-1047; SQ-9993
Routes of
administration		Intramuscular injection[1]
Drug classEstrogen; Estrogen ester
ATC code
Legal status
Legal status
  • In general: ℞ (Prescription only)
Pharmacokinetic data
BioavailabilityIM injection: High
Protein bindingEstradiol: ~98% (to albumin and SHBG)[2][3]
MetabolismCleavage via esterases in the liver, blood, and tissues[4][5]
MetabolitesEstradiol, undecanoic acid, estradiol metabolites[4][5]
Elimination half-lifeUnknown
Duration of actionIM injection:
• 10–12.5 mg: 1–2 months[6][7]
• 25–50 mg: 2–4 months[8]
ExcretionUrine
Identifiers
  • [(8R,9S,13S,14S,17S)-3-hydroxy-13-methyl-6,7,8,9,11,12,14,15,16,17-decahydrocyclopenta[a]phenanthren-17-yl] undecanoate
CAS Number
  • 3571-53-7 Y
PubChem CID
  • 19135
ChemSpider
  • 18055
UNII
  • H3N3A8MFJC
KEGG
  • D04065
ChEMBL
  • ChEMBL1697794
CompTox Dashboard (EPA)
  • DTXSID3023003
ECHA InfoCard100.020.616
Chemical and physical data
FormulaC29H44O3
Molar mass440.668 g·mol−1
3D model (JSmol)
  • Interactive image
  • CCCCCCCCCCC(=O)O[C@H]1CC[C@@H]2[C@@]1(CC[C@H]3[C@H]2CCC4=C3C=CC(=C4)O)C
  • InChI=1S/C29H44O3/c1-3-4-5-6-7-8-9-10-11-28(31)32-27-17-16-26-25-14-12-21-20-22(30)13-15-23(21)24(25)18-19-29(26,27)2/h13,15,20,24-27,30H,3-12,14,16-19H2,1-2H3/t24-,25-,26+,27+,29+/m1/s1
  • Key:TXHUMRBWIWWBGW-GVGNIZHQSA-N

Side effects of estradiol undecylate in men may include breast tenderness, breast development, feminization, sexual dysfunction, infertility, fluid retention, and cardiovascular issues.[17] Estradiol undecylate is an estrogen and hence is an agonist of the estrogen receptor, the biological target of estrogens like estradiol.[5][4] It is an estrogen ester and a very long-lasting prodrug of estradiol in the body.[4][5] Because of this, it is considered to be a natural and bioidentical form of estrogen.[4][18][19] An injection of estradiol undecylate has a duration of about 1 to 4 months.[7][8][6][20]

Estradiol undecylate was first described in 1953 and was introduced for medical use by 1956.[7][21][8][22] It remained in use as late as the 2000s before being discontinued.[23][11][24] Estradiol undecylate was marketed in Europe, but does not seem to have ever been available in the United States.[14][25][11] It was used for many years as a parenteral estrogen to treat prostate cancer in men, although it was not employed as often as polyestradiol phosphate.[12]

Medical uses Edit

Main article: Estradiol (medication) § Medical uses

Estradiol undecylate has been used as a form of high-dose estrogen therapy to treat prostate cancer, but has since largely been superseded for this indication by newer agents with fewer adverse effects (e.g., gynecomastia and cardiovascular complications) like GnRH analogues and nonsteroidal antiandrogens.[1][26] It has been assessed for this purpose in a number of clinical studies.[27][28][29][30][31] It has been used at a dosage of 100 mg every 3 to 4 weeks (or once a month) by intramuscular injection for this indication.[17][32]

Estradiol undecylate has been used to suppress sex drive in sex offenders.[33] It has been used for this indication at a dosage of 50 to 100 mg by intramuscular injection once every 3 to 4 weeks.[33]

Estradiol undecylate has also been used to treat breast cancer in women.[34] It has been used in menopausal hormone therapy as well, for instance in the treatment of hot flashes and other menopausal symptoms.[8] Along with estradiol valerate, estradiol cypionate, and estradiol benzoate, estradiol undecylate has been used as an intramuscular estrogen in feminizing hormone therapy for transgender women.[13][14][15] It has been used at doses of 100 to as much as 800 mg per month by intramuscular injection for this purpose.[14][15][13][35][36][37]

Estrogen dosages for prostate cancer
Route/form Estrogen Dosage
Oral Estradiol 1–2 mg 3x/day
Conjugated estrogens 1.25–2.5 mg 3x/day
Ethinylestradiol 0.15–3 mg/day
Ethinylestradiol sulfonate 1–2 mg 1x/week
Diethylstilbestrol 1–3 mg/day
Dienestrol 5 mg/day
Hexestrol 5 mg/day
Fosfestrol 100–480 mg 1–3x/day
Chlorotrianisene 12–48 mg/day
Quadrosilan 900 mg/day
Estramustine phosphate 140–1400 mg/day
Transdermal patch Estradiol 2–6x 100 μg/day
Scrotal: 1x 100 μg/day
IM or SC injection Estradiol benzoate 1.66 mg 3x/week
Estradiol dipropionate 5 mg 1x/week
Estradiol valerate 10–40 mg 1x/1–2 weeks
Estradiol undecylate 100 mg 1x/4 weeks
Polyestradiol phosphate Alone: 160–320 mg 1x/4 weeks
With oral EE: 40–80 mg 1x/4 weeks
Estrone 2–4 mg 2–3x/week
IV injection Fosfestrol 300–1200 mg 1–7x/week
Estramustine phosphate 240–450 mg/day
Note: Dosages are not necessarily equivalent. Sources: See template.

Available forms Edit

Estradiol undecylate was available as an oil solution for intramuscular injection provided in ampoules at a concentration of 100 mg/mL.[23][38]

Contraindications Edit

See also: Estradiol (medication) § Contraindications

Contraindications of estrogens include coagulation problems, cardiovascular diseases, liver disease, and certain hormone-sensitive cancers such as breast cancer and endometrial cancer, among others.[39][40][41][42]

Side effects Edit

Main article: Estradiol (medication) § Side effects

Estradiol undecylate and its side effects have been evaluated for the treatment of advanced prostate cancer in a phase III international multicenter randomized controlled trial headed by Jacobi and colleagues of the Department of Urology, University of Mainz.[17][43][44][45][46][28][47] The study consisted of 191 patients from 12 treatment centers, who were treated for 6 months with intramuscular injections of either 100 mg/month estradiol undecylate (96 men) or 300 mg/week cyproterone acetate (95 men).[43][45][46][28][47][48][49] Findings for a subgroup of 42 men at the University of Mainz center were initially reported in 1978 and 1980.[50][17][28][47] These men were age 51 to 84 years (mean 68 years), and men with pre-existing cardiovascular disease were excluded.[12][17][51] A considerable incidence of cardiovascular complications was reported for the estradiol undecylate group (76%; 16/21 incidence total); there was a 67% (14/21) incidence of cardiovascular morbidity and a 9.5% (2/21) incidence of cardiovascular mortality.[12][17][51] The cardiovascular morbidity in this group included peripheral edema and superficial thrombophlebitis (38%; 8/21), coronary heart disease (24%; 5/21), and a deep vein thrombosis (4.8%; 1/21), while the cardiovascular mortality included a myocardial infarction (4.8%; 1/21) and a pulmonary embolism (4.8%; 1/21).[17][51] Eight of the cases of cardiovascular complications in the estradiol undecylate group, including the two deaths, were regarded as "severe".[51][52] Conversely, no incidence of cardiovascular toxicity occurred in the cyproterone acetate comparison group (0%; 0/21).[12][17][51] Other side effects of estradiol undecylate included gynecomastia (100%; 21/21) and erectile dysfunction (90%; 19/21).[17] The cardiovascular complications with estradiol undecylate in this relatively small study are in contrast to large and high-quality clinical studies of high-dose polyestradiol phosphate and transdermal estradiol for prostate cancer, in which minimal to no cardiovascular toxicity has been observed.[53][54][55][56][57]

An expanded report of 191 patients, which included the 42 patients from the University of Mainz center plus an additional 149 patients from 11 other centers, was published in 1982.[43][49] The antitumor effectiveness of estradiol undecylate and cyproterone acetate in this study was equivalent.[43][45][58][46][28][47] The rates of improvement, no response, and deterioration were 52%, 41%, and 7% in the estradiol undecylate group and 48%, 44%, and 8% in the cyproterone acetate group, respectively.[43][46] However, the incidence of a selection of specific side effects, including gynecomastia, breast tenderness, and edema, was significantly lower in the cyproterone acetate group than in the estradiol undecylate group (37% vs. 94%, respectively).[43][45][46][59] Gynecomastia specifically occurred in 13% (12/96) of the patients in the cyproterone acetate group and 77% (73/95) of the patients in the estradiol undecylate group.[43][45] Erectile dysfunction occurred in "essentially all" patients in both groups.[49] Leg edema occurred in 18% (17/95) of the estradiol undecylate group and 4.2% (4/96) of the cyproterone acetate group, while the incidences of superficial thrombophlebitis and coronary heart disease both were not described.[43] The incidence of thrombosis was 4.2% (4/95) in the estradiol undecylate group and 5.3% (5/96) in the cyproterone acetate group.[43][48][49] There were five deaths in total, three in the estradiol undecylate group and two in the cyproterone acetate group.[43] Two of the deaths in each of the treatment groups were due to cardiovascular events, while the remaining death in the estradiol undecylate group was due to unknown causes.[43][46][49] The similar rate of cardiovascular complications besides edema between estradiol undecylate and cyproterone acetate that was observed is in contrast to the initial 42-patient report and to findings with other estrogens, such as diethylstilbestrol and estramustine phosphate, which have been shown to possess significantly higher cardiovascular toxicity than cyproterone acetate.[45] On the basis of the expanded study, the researchers concluded that cyproterone acetate was an "acceptable alternative" to estrogen therapy with estradiol undecylate, but with a "considerably more favorable" side-effect profile.[46]

After the completion of the initial expanded study, a 5-year extension trial primarily of the Ruhr University Bochum center subgroup, led by Tunn and colleagues, was conducted.[29][44][45][28][48][47] In this study, the cyproterone acetate group was changed from intramuscular injections to 100 mg/day oral cyproterone acetate.[29][45] Of the 39 patients in the study, the global 5-year survival rate was not significantly different between the estradiol undecylate and cyproterone acetate groups (24% and 26%, respectively).[29][45][28][48][47] In patients without metastases, the 5-year survival rate was 51% in the cyproterone acetate group relative to 43% in the estradiol undecylate group, although the difference was not statistically significant.[29][45] In terms of non-prostate cancer deaths, there were 5 in the CPA group and 6 in the EU group.[29] The incidence of cardiovascular-related mortality was 3 deaths in the CPA group and 3 deaths in the EU group.[29]

Side effects of estradiol undecylate versus cyproterone acetate in men
Side effect Estradiol undecylate
100 mg/month i.m. (n = 96)		 Cyproterone acetate
100 mg/day oral (n = 95)
n % n %
Gynecomastia* 74 77.1% 12 12.6%
Breast tenderness* 84 87.5% 6 6.3%
Sexual impotence
"Occurred in essentially all patients of both groups"
Leg edema* 17 17.7% 4 4.2%
Thrombosis 4 4.2% 5 5.3%
Cardiovascular mortality 2 2.1% 2 2.1%
Other mortality 1a 1.0% 0 0%
Notes: For 6 months in 191 men age 51 to 88 years with prostate cancer. Footnotes: * = Differences in incidences between groups were statistically significant. a = Due to unknown causes. Sources: See template.

The side effects of estradiol undecylate have also been studied and reported beyond the preceding clinical trial programme and for other patient populations, for instance women. Side effects during therapy with massive doses of estradiol undecylate (200 mg three times per week, or 600 mg per week and around 2,400 mg per month total) in postmenopausal women with advanced breast cancer have included appetite loss, nausea, vomiting, vaginal bleeding, vaginal discharge, nipple pigmentation, breast pain, rash, urinary incontinence, edema, drowsiness, hypercalcemia, and local injection-site reactions.[34] Like with other estrogens, treatment with estradiol undecylate has been found to produce testicular abnormalities and disturbances of spermatogenesis in men.[60] In transgender women, estradiol undecylate by intramuscular injection at extremely high doses (200–800 mg/month) was associated with greater incidence of hyperprolactinemia (high prolactin levels) than ethinylestradiol orally at a dose of 100 μg/day (or about 3 mg/month total) (rates of 40% and 16% for prolactin levels greater than 1,000 mU/L, respectively).[35] Switching from estradiol undecylate to ethinylestradiol resulted in a decrease in prolactin levels in many individuals.[35] The preceding dosage of estradiol undecylate corresponds to much greater estrogenic exposure than the dosage of ethinylestradiol.[35] Cyproterone acetate was also used in combination with estrogen in the study.[35]

Overdose Edit

See also: Estradiol (medication) § Overdose

Estradiol undecylate has been used clinically at massive doses of as much as 800 to 2,400 mg per month by intramuscular injection, given in divided doses of 100 to 200 mg per injection two to three times per week.[34][15][35][36][37] For purposes of comparison, a single 100 mg intramuscular injection of estradiol undecylate has been reported to produce estradiol levels of about 500 pg/mL.[61] Symptoms of estrogen overdosage may include nausea, vomiting, bloating, increased weight, water retention, breast tenderness, vaginal discharge, heavy legs, and leg cramps.[39] These side effects can be diminished by reducing the estrogen dosage.[39]

Interactions Edit

See also: Estradiol (medication) § Interactions

Inhibitors and inducers of cytochrome P450 may influence the metabolism of estradiol and by extension circulating estradiol levels.[62]

Pharmacology Edit

 
Estradiol, the active form of estradiol undecylate.

Pharmacodynamics Edit

See also: Pharmacodynamics of estradiol

Esters of estradiol like estradiol undecylate are readily hydrolyzed prodrugs of estradiol, but have an extended duration when administered in oil via intramuscular injection due to a depot effect afforded by their fatty acid ester moiety.[5] As prodrugs of estradiol, estradiol undecylate and other estradiol esters are estrogens.[4][5] Estradiol undecylate is of about 62% higher molecular weight than estradiol due to the presence of its C17β undecylate ester.[9][11] Because estradiol undecylate is a prodrug of estradiol, it is considered to be a natural and bioidentical form of estrogen.[4][18][19]

The effects of estradiol undecylate on cortisol, dehydroepiandrosterone sulfate, testosterone, prolactin, and sex hormone-binding globulin levels as well as on the hypothalamic–pituitary–adrenal axis have been studied in men with prostate cancer and compared with those of high-dose cyproterone acetate therapy.[63][64][65][66][67][17][68][69][70][71] The effects of estradiol undecylate on serum lipids and ceruloplasmin levels have been studied as well.[72][73][74] Additionally, the influence of estradiol undecylate on SHBG levels and free testosterone fraction in women has been described.[75]

Potencies and durations of natural estrogens by intramuscular injection
Estrogen Form Dose (mg) Duration by dose (mg)
EPD CICD
Estradiol Aq. soln. ? <1 d
Oil soln. 40–60 1–2 ≈ 1–2 d
Aq. susp. ? 3.5 0.5–2 ≈ 2–7 d; 3.5 ≈ >5 d
Microsph. ? 1 ≈ 30 d
Estradiol benzoate Oil soln. 25–35 1.66 ≈ 2–3 d; 5 ≈ 3–6 d
Aq. susp. 20 10 ≈ 16–21 d
Emulsion ? 10 ≈ 14–21 d
Estradiol dipropionate Oil soln. 25–30 5 ≈ 5–8 d
Estradiol valerate Oil soln. 20–30 5 5 ≈ 7–8 d; 10 ≈ 10–14 d;
40 ≈ 14–21 d; 100 ≈ 21–28 d
Estradiol benz. butyrate Oil soln. ? 10 10 ≈ 21 d
Estradiol cypionate Oil soln. 20–30 5 ≈ 11–14 d
Aq. susp. ? 5 5 ≈ 14–24 d
Estradiol enanthate Oil soln. ? 5–10 10 ≈ 20–30 d
Estradiol dienanthate Oil soln. ? 7.5 ≈ >40 d
Estradiol undecylate Oil soln. ? 10–20 ≈ 40–60 d;
25–50 ≈ 60–120 d
Polyestradiol phosphate Aq. soln. 40–60 40 ≈ 30 d; 80 ≈ 60 d;
160 ≈ 120 d
Estrone Oil soln. ? 1–2 ≈ 2–3 d
Aq. susp. ? 0.1–2 ≈ 2–7 d
Estriol Oil soln. ? 1–2 ≈ 1–4 d
Polyestriol phosphate Aq. soln. ? 50 ≈ 30 d; 80 ≈ 60 d
Notes and sources
Notes: All aqueous suspensions are of microcrystalline particle size. Estradiol production during the menstrual cycle is 30–640 µg/d (6.4–8.6 mg total per month or cycle). The vaginal epithelium maturation dosage of estradiol benzoate or estradiol valerate has been reported as 5 to 7 mg/week. An effective ovulation-inhibiting dose of estradiol undecylate is 20–30 mg/month. Sources: See template.

Antigonadotropic activity Edit

 
Testosterone levels with 300 mg/week cyproterone acetate or 100 mg/month estradiol undecylate both by intramuscular injection.[17] The solid lines are the average levels and the dashed lines are the highest and lowest observed levels.
 
Estradiol, testosterone, and prolactin levels with 100 mg/month estradiol undecylate by intramuscular injection in men with prostate cancer.[65]

A phase III clinical trial comparing high-dose intramuscular cyproterone acetate (300 mg/week) and high-dose intramuscular estradiol undecylate (100 mg/month) in the treatment of prostate cancer found that estradiol undecylate suppressed testosterone levels into the castrate range (< 50 ng/dL)[76] within at least 3 months whereas testosterone levels with cyproterone acetate were significantly higher and above the castrate range even after 6 months of treatment.[17] With estradiol undecylate, testosterone levels fell from 416 ng/dL to 38 ng/mL (–91%) after 3 months and to 29.6 ng/dL (–93%) after 6 months, whereas with cyproterone acetate, testosterone levels fell from 434 ng/dL to 107 ng/mL (–75%) at 3 months and to 102 ng/mL (–76%) at 6 months.[17] In another study using the same dosages, estradiol undecylate suppressed testosterone levels by 97% while CPA suppressed them by 70%.[67] In accordance, whereas estrogens are well-established as able to suppress testosterone levels into the castrate range at sufficiently high dosages,[77] progestogens like cyproterone acetate on their own are able to decrease testosterone levels only up to an apparent maximum of around 70 to 80%.[78][79] Besides effects on testosterone levels, the long-term effects of estradiol undecylate on testicular morphology in transgender women have been studied.[60]

Pharmacokinetics Edit

See also: Pharmacokinetics of estradiol

The pharmacokinetics of estradiol undecylate have been assessed limitedly in a few studies.[80][81][82][83][65][84][7][8] Following a single intramuscular injection of 100 mg estradiol undecylate in oil, mean levels of estradiol were about 500 pg/mL a day after injection and about 340 pg/mL 14 days after injection in 4 people.[80] Levels of estradiol with intramuscular estradiol undecylate were reported to be very irregular and to vary by as much as 10-fold between individuals.[80] In another study, following a single intramuscular injection of 32.2 mg estradiol undecylate, levels of estradiol peaked at around 400 pg/mL after 3 days and decreased from this peak to around 200 pg/mL after 6 days in 3 postmenopausal women.[81][85] In a repeated administration study of 100 mg per month estradiol undecylate in 14 men with prostate cancer, estradiol levels at trough were about 560 pg/mL at 3 months and about 540 pg/mL at 6 months following initiation of therapy.[65] In a larger follow-up of the study with 21 men, estradiol levels at trough were about 36 pg/mL at baseline, 486 pg/mL at 3 months, and 598 pg/mL at 6 months of therapy.[70] In one further study, levels of estradiol in an unspecified number of postmenopausal women following a single injection of 100 mg estradiol undecylate were said to be between 300 pg/mL and 600 pg/mL six days post-injection.[75]

Due to its more protracted duration, doses of estradiol undecylate that are typical of other estradiol esters produce only "subthreshold" estradiol levels, and for this reason, higher single doses of estradiol undecylate are necessary for similar effects.[86][80][81] However, the relatively low levels of estradiol produced by lower doses of estradiol undecylate are favorable for menopausal replacement therapy.[86]

The duration of estradiol undecylate is markedly prolonged relative to that of estradiol benzoate, estradiol valerate, and many other estradiol esters.[61][6][20][18] A single intramuscular injection of 10 to 12.5 mg estradiol undecylate has a duration of 40 to 60 days (~1–2 months) and of 25 to 50 mg estradiol undecylate has an estimated duration of effect of 2 to 4 months in postmenopausal women.[7][8][6][20] A single intramuscular injection of 20 to 30 mg estradiol undecylate has been found to inhibit ovulation when used as an estrogen-only injectable contraceptive in premenopausal women for 1 to 3 months (mean 1.7 months) as well.[87] When used at a higher dose of 100 mg per injection in men with prostate cancer, estradiol undecylate has been given usually once a month.[17][32] After a single subcutaneous injection of estradiol undecylate in rats, its duration of effect was 80 days (about 2.5 months).[88][89][90] Due to its very prolonged duration, estradiol undecylate has been described in general as a favorable alternative to estradiol implants.[8]

The excretion of estradiol undecylate has been studied as well.[83]

Estradiol undecylate has not been used via oral administration. However, a closely related estradiol ester, estradiol decanoate (estradiol decylate), has been studied via the oral route, and has been found to possess significant oral bioavailability, to produce relatively high estradiol levels of about 100 pg/mL after a single 0.5 mg oral dose and about 100 to 150 pg/mL with continuous 0.25 mg/day oral therapy, and to have a much higher estradiol-to-estrone ratio than oral estradiol of about 2:1.[91][92][93] It is thought that this is due to absorption of estradiol decanoate by the lymphatic system and a consequent partial bypass of first-pass metabolism in the liver and intestines,[91][92][93] which is similarly known to occur with oral testosterone undecanoate.[94][95]

Hormone levels with estradiol undecylate by intramuscular injection

Chemistry Edit

See also: Estrogen ester and List of estrogen esters § Estradiol esters

Estradiol undecylate is a synthetic estrane steroid and an estradiol ester.[9][10] It is specifically the C17β undecylate (undecanoate) ester of estradiol.[9][10][11] The compound is also known as estradiol 17β-undecylate or as estra-1,3,5(10)-triene-3,17β-diol 17β-undecanoate.[10][11] The undecylic acid (undecanoic acid) ester of estradiol undecylate is a medium-chain fatty acid and is found naturally in many foods, some examples of which include coconut, fruits, fats, oils, and rice.[97]

Estradiol undecylate is a relatively long-chain ester of estradiol.[10][11] Its undecylate ester contains 11 carbon atoms.[10][11] For comparison, the ester chains of estradiol acetate, estradiol valerate, and estradiol enantate have 2, 5, and 7 carbon atoms, respectively.[10][11] As a result of its longer ester chain, estradiol undecylate is the most lipophilic of these estradiol esters, and for this reason, has by far the longest duration when administered in oil solution by intramuscular injection.[61][98][99] An example of an estradiol ester with a longer ester chain than estradiol undecylate is estradiol stearate (Depofollan), which has 18 carbon atoms and has been used in medicine as an estrogen as well.

A few estradiol esters related to estradiol undecylate include estradiol decanoate, estradiol diundecylate, and estradiol diundecylenate.[9][10] Estradiol undecylate shares the same undecylate ester as testosterone undecanoate, an androgen/anabolic steroid and very long-lasting testosterone ester.[9][10]

Estradiol undecylate is one of the longest-chain steroid esters that has been in common medical use.[100]

Structural properties of selected estradiol esters
Estrogen Structure Ester(s) Relative
mol. weight		 Relative
E2 contentb		 log Pc
Position(s) Moiet(ies) Type Lengtha
Estradiol
 
 1.00 1.00 4.0
Estradiol acetate
 
 C3 Ethanoic acid Straight-chain fatty acid 2 1.15 0.87 4.2
Estradiol benzoate
 
 C3 Benzenecarboxylic acid Aromatic fatty acid – (~4–5) 1.38 0.72 4.7
Estradiol dipropionate
 
 C3, C17β Propanoic acid (×2) Straight-chain fatty acid 3 (×2) 1.41 0.71 4.9
Estradiol valerate
 
 C17β Pentanoic acid Straight-chain fatty acid 5 1.31 0.76 5.6–6.3
Estradiol benzoate butyrate
 
 C3, C17β Benzoic acid, butyric acid Mixed fatty acid – (~6, 2) 1.64 0.61 6.3
Estradiol cypionate
 
 C17β Cyclopentylpropanoic acid Aromatic fatty acid – (~6) 1.46 0.69 6.9
Estradiol enanthate
 
 C17β Heptanoic acid Straight-chain fatty acid 7 1.41 0.71 6.7–7.3
Estradiol dienanthate
 
 C3, C17β Heptanoic acid (×2) Straight-chain fatty acid 7 (×2) 1.82 0.55 8.1–10.4
Estradiol undecylate
 
 C17β Undecanoic acid Straight-chain fatty acid 11 1.62 0.62 9.2–9.8
Estradiol stearate
 
 C17β Octadecanoic acid Straight-chain fatty acid 18 1.98 0.51 12.2–12.4
Estradiol distearate
 
 C3, C17β Octadecanoic acid (×2) Straight-chain fatty acid 18 (×2) 2.96 0.34 20.2
Estradiol sulfate
 
 C3 Sulfuric acid Water-soluble conjugate 1.29 0.77 0.3–3.8
Estradiol glucuronide
 
 C17β Glucuronic acid Water-soluble conjugate 1.65 0.61 2.1–2.7
Estramustine phosphated
 
 C3, C17β Normustine, phosphoric acid Water-soluble conjugate 1.91 0.52 2.9–5.0
Polyestradiol phosphatee
 
 C3–C17β Phosphoric acid Water-soluble conjugate 1.23f 0.81f 2.9g
Footnotes: a = Length of ester in carbon atoms for straight-chain fatty acids or approximate length of ester in carbon atoms for aromatic fatty acids. b = Relative estradiol content by weight (i.e., relative estrogenic exposure). c = Experimental or predicted octanol/water partition coefficient (i.e., lipophilicity/hydrophobicity). Retrieved from PubChem, ChemSpider, and DrugBank. d = Also known as estradiol normustine phosphate. e = Polymer of estradiol phosphate (~13 repeat units). f = Relative molecular weight or estradiol content per repeat unit. g = log P of repeat unit (i.e., estradiol phosphate). Sources: See individual articles.

History Edit

Estradiol undecylate was first described in the scientific literature, along with estradiol valerate and a variety of other estradiol esters, by Karl Junkmann of Schering AG in 1953.[101][7] It was introduced for medical use via intramuscular injection by 1956.[21][8][22] Syntex applied for a patent for estradiol undecylate in 1958, which was granted in 1961 and was given a priority date of 1957.[23][102] Estradiol undecylate was introduced for medical use and was employed for decades, but was eventually discontinued.[11][25][38] It remained in use in some countries as late as the 2000s.[23][11][24]

Harry Benjamin reported on the use of estradiol undecylate in transgender women in his book The Transsexual Phenomenon in 1966 and in a literature review in the Journal of Sex Research in 1967.[14][103]

Society and culture Edit

Generic names Edit

Estradiol undecylate is the generic name of the drug and its INN and USAN.[9][10][11][16] It is also spelled in some publications as estradiol unducelate and is also known as estradiol undecanoate.[61][9][10][11][16] In German, it is known under a variety of spellings including as estradiolundecylat, östradiolundecylat, östradiolundezylat, oestradiolundecylat, oestradiolundezylat, and others.[104] Estradiol undecylate is known by its former developmental code names RS-1047 and SQ-9993 as well.[9][10][11][16]

Brand names Edit

The major brand name of estradiol undecylate is Progynon Depot 100.[9][10][11] It has also been marketed under other brand names including Delestrec, Depogin, Estrolent, Oestradiol D, Oestradiol-Retard Theramex, and Primogyn Depot [0,1 mg/ml], among others.[9][10][11][23][24]

Availability Edit

Estradiol undecylate was available in the Europe (including in France, Germany, Great Britain, Monaco, the Netherlands, Switzerland), and Japan.[11][23][105][22][106] However, it has been discontinued and hence is no longer available.[25][38]

Research Edit

Estradiol undecylate was studied by Schering alone as an estrogen-only injectable contraceptive in premenopausal women at a dose of 20 to 30 mg once a month.[85][87][107][108] It was effective, lacked breast and thromboembolic complications, lacked other side effects besides amenorrhea, and prevented ovulation for 1 to 3 months (mean 1.7 months) following a single dose.[87] However, uterine growth of 1 to 2 cm was observed after one year, and endometrial hyperplasia was occasionally encountered.[85][87][107] The preparation was not further developed as a form of birth control due to the risks of endometrial hyperplasia and cancer associated with long-term unopposed estrogen therapy.[87]

Estradiol undecylate, in combination with norethisterone enanthate (at doses of 5 to 10 mg and 50 to 70 mg, respectively), was studied by Schering as a combined injectable contraceptive in premenopausal women and was found to be effective and well-tolerated, but ultimately was not marketed for this use.[109][108][87][110][111][112]

See also Edit

References Edit

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August 27, 2023
estradiol, undecylate, also, known, estradiol, undecanoate, formerly, sold, under, brand, names, delestrec, progynon, depot, among, others, estrogen, medication, which, been, used, treatment, prostate, cancer, also, been, used, part, hormone, therapy, transgen. Estradiol undecylate EU or E2U also known as estradiol undecanoate and formerly sold under the brand names Delestrec and Progynon Depot 100 among others is an estrogen medication which has been used in the treatment of prostate cancer in men 9 10 11 12 1 It has also been used as a part of hormone therapy for transgender women 13 14 15 Although estradiol undecylate has been used in the past it was discontinued and hence is no longer available 11 16 The medication has been given by injection into muscle usually once a month 1 17 12 Estradiol undecylateClinical dataPronunciation ˌ ɛ s t r e ˈ d aɪ ɒ l e n ˈ d ɛ s ɪ l eɪ t ES tre DY ol un DESS il aytTrade namesDelestrec Progynon Depot 100 othersOther namesEU E2U Estradiol undecanoate Estradiol unducelate RS 1047 SQ 9993Routes ofadministrationIntramuscular injection 1 Drug classEstrogen Estrogen esterATC codeG03CA03 WHO Legal statusLegal statusIn general Prescription only Pharmacokinetic dataBioavailabilityIM injection HighProtein bindingEstradiol 98 to albumin and SHBG 2 3 MetabolismCleavage via esterases in the liver blood and tissues 4 5 MetabolitesEstradiol undecanoic acid estradiol metabolites 4 5 Elimination half lifeUnknownDuration of actionIM injection 10 12 5 mg 1 2 months 6 7 25 50 mg 2 4 months 8 ExcretionUrineIdentifiersIUPAC name 8R 9S 13S 14S 17S 3 hydroxy 13 methyl 6 7 8 9 11 12 14 15 16 17 decahydrocyclopenta a phenanthren 17 yl undecanoateCAS Number3571 53 7 YPubChem CID19135ChemSpider18055UNIIH3N3A8MFJCKEGGD04065ChEMBLChEMBL1697794CompTox Dashboard EPA DTXSID3023003ECHA InfoCard100 020 616Chemical and physical dataFormulaC 29H 44O 3Molar mass440 668 g mol 13D model JSmol Interactive imageSMILES CCCCCCCCCCC O O C H 1CC C H 2 C 1 CC C H 3 C H 2CCC4 C3C CC C4 O CInChI InChI 1S C29H44O3 c1 3 4 5 6 7 8 9 10 11 28 31 32 27 17 16 26 25 14 12 21 20 22 30 13 15 23 21 24 25 18 19 29 26 27 2 h13 15 20 24 27 30H 3 12 14 16 19H2 1 2H3 t24 25 26 27 29 m1 s1Key TXHUMRBWIWWBGW GVGNIZHQSA NSide effects of estradiol undecylate in men may include breast tenderness breast development feminization sexual dysfunction infertility fluid retention and cardiovascular issues 17 Estradiol undecylate is an estrogen and hence is an agonist of the estrogen receptor the biological target of estrogens like estradiol 5 4 It is an estrogen ester and a very long lasting prodrug of estradiol in the body 4 5 Because of this it is considered to be a natural and bioidentical form of estrogen 4 18 19 An injection of estradiol undecylate has a duration of about 1 to 4 months 7 8 6 20 Estradiol undecylate was first described in 1953 and was introduced for medical use by 1956 7 21 8 22 It remained in use as late as the 2000s before being discontinued 23 11 24 Estradiol undecylate was marketed in Europe but does not seem to have ever been available in the United States 14 25 11 It was used for many years as a parenteral estrogen to treat prostate cancer in men although it was not employed as often as polyestradiol phosphate 12 Contents 1 Medical uses 1 1 Available forms 2 Contraindications 3 Side effects 4 Overdose 5 Interactions 6 Pharmacology 6 1 Pharmacodynamics 6 1 1 Antigonadotropic activity 6 2 Pharmacokinetics 7 Chemistry 8 History 9 Society and culture 9 1 Generic names 9 2 Brand names 9 3 Availability 10 Research 11 See also 12 ReferencesMedical uses EditMain article Estradiol medication Medical uses Estradiol undecylate has been used as a form of high dose estrogen therapy to treat prostate cancer but has since largely been superseded for this indication by newer agents with fewer adverse effects e g gynecomastia and cardiovascular complications like GnRH analogues and nonsteroidal antiandrogens 1 26 It has been assessed for this purpose in a number of clinical studies 27 28 29 30 31 It has been used at a dosage of 100 mg every 3 to 4 weeks or once a month by intramuscular injection for this indication 17 32 Estradiol undecylate has been used to suppress sex drive in sex offenders 33 It has been used for this indication at a dosage of 50 to 100 mg by intramuscular injection once every 3 to 4 weeks 33 Estradiol undecylate has also been used to treat breast cancer in women 34 It has been used in menopausal hormone therapy as well for instance in the treatment of hot flashes and other menopausal symptoms 8 Along with estradiol valerate estradiol cypionate and estradiol benzoate estradiol undecylate has been used as an intramuscular estrogen in feminizing hormone therapy for transgender women 13 14 15 It has been used at doses of 100 to as much as 800 mg per month by intramuscular injection for this purpose 14 15 13 35 36 37 vte Estrogen dosages for prostate cancer Route form Estrogen DosageOral Estradiol 1 2 mg 3x dayConjugated estrogens 1 25 2 5 mg 3x dayEthinylestradiol 0 15 3 mg dayEthinylestradiol sulfonate 1 2 mg 1x weekDiethylstilbestrol 1 3 mg dayDienestrol 5 mg dayHexestrol 5 mg dayFosfestrol 100 480 mg 1 3x dayChlorotrianisene 12 48 mg dayQuadrosilan 900 mg dayEstramustine phosphate 140 1400 mg dayTransdermal patch Estradiol 2 6x 100 mg dayScrotal 1x 100 mg dayIM or SC injection Estradiol benzoate 1 66 mg 3x weekEstradiol dipropionate 5 mg 1x weekEstradiol valerate 10 40 mg 1x 1 2 weeksEstradiol undecylate 100 mg 1x 4 weeksPolyestradiol phosphate Alone 160 320 mg 1x 4 weeksWith oral EE 40 80 mg 1x 4 weeksEstrone 2 4 mg 2 3x weekIV injection Fosfestrol 300 1200 mg 1 7x weekEstramustine phosphate 240 450 mg dayNote Dosages are not necessarily equivalent Sources See template Available forms Edit Estradiol undecylate was available as an oil solution for intramuscular injection provided in ampoules at a concentration of 100 mg mL 23 38 Contraindications EditSee also Estradiol medication Contraindications Contraindications of estrogens include coagulation problems cardiovascular diseases liver disease and certain hormone sensitive cancers such as breast cancer and endometrial cancer among others 39 40 41 42 Side effects EditMain article Estradiol medication Side effects Estradiol undecylate and its side effects have been evaluated for the treatment of advanced prostate cancer in a phase III international multicenter randomized controlled trial headed by Jacobi and colleagues of the Department of Urology University of Mainz 17 43 44 45 46 28 47 The study consisted of 191 patients from 12 treatment centers who were treated for 6 months with intramuscular injections of either 100 mg month estradiol undecylate 96 men or 300 mg week cyproterone acetate 95 men 43 45 46 28 47 48 49 Findings for a subgroup of 42 men at the University of Mainz center were initially reported in 1978 and 1980 50 17 28 47 These men were age 51 to 84 years mean 68 years and men with pre existing cardiovascular disease were excluded 12 17 51 A considerable incidence of cardiovascular complications was reported for the estradiol undecylate group 76 16 21 incidence total there was a 67 14 21 incidence of cardiovascular morbidity and a 9 5 2 21 incidence of cardiovascular mortality 12 17 51 The cardiovascular morbidity in this group included peripheral edema and superficial thrombophlebitis 38 8 21 coronary heart disease 24 5 21 and a deep vein thrombosis 4 8 1 21 while the cardiovascular mortality included a myocardial infarction 4 8 1 21 and a pulmonary embolism 4 8 1 21 17 51 Eight of the cases of cardiovascular complications in the estradiol undecylate group including the two deaths were regarded as severe 51 52 Conversely no incidence of cardiovascular toxicity occurred in the cyproterone acetate comparison group 0 0 21 12 17 51 Other side effects of estradiol undecylate included gynecomastia 100 21 21 and erectile dysfunction 90 19 21 17 The cardiovascular complications with estradiol undecylate in this relatively small study are in contrast to large and high quality clinical studies of high dose polyestradiol phosphate and transdermal estradiol for prostate cancer in which minimal to no cardiovascular toxicity has been observed 53 54 55 56 57 An expanded report of 191 patients which included the 42 patients from the University of Mainz center plus an additional 149 patients from 11 other centers was published in 1982 43 49 The antitumor effectiveness of estradiol undecylate and cyproterone acetate in this study was equivalent 43 45 58 46 28 47 The rates of improvement no response and deterioration were 52 41 and 7 in the estradiol undecylate group and 48 44 and 8 in the cyproterone acetate group respectively 43 46 However the incidence of a selection of specific side effects including gynecomastia breast tenderness and edema was significantly lower in the cyproterone acetate group than in the estradiol undecylate group 37 vs 94 respectively 43 45 46 59 Gynecomastia specifically occurred in 13 12 96 of the patients in the cyproterone acetate group and 77 73 95 of the patients in the estradiol undecylate group 43 45 Erectile dysfunction occurred in essentially all patients in both groups 49 Leg edema occurred in 18 17 95 of the estradiol undecylate group and 4 2 4 96 of the cyproterone acetate group while the incidences of superficial thrombophlebitis and coronary heart disease both were not described 43 The incidence of thrombosis was 4 2 4 95 in the estradiol undecylate group and 5 3 5 96 in the cyproterone acetate group 43 48 49 There were five deaths in total three in the estradiol undecylate group and two in the cyproterone acetate group 43 Two of the deaths in each of the treatment groups were due to cardiovascular events while the remaining death in the estradiol undecylate group was due to unknown causes 43 46 49 The similar rate of cardiovascular complications besides edema between estradiol undecylate and cyproterone acetate that was observed is in contrast to the initial 42 patient report and to findings with other estrogens such as diethylstilbestrol and estramustine phosphate which have been shown to possess significantly higher cardiovascular toxicity than cyproterone acetate 45 On the basis of the expanded study the researchers concluded that cyproterone acetate was an acceptable alternative to estrogen therapy with estradiol undecylate but with a considerably more favorable side effect profile 46 After the completion of the initial expanded study a 5 year extension trial primarily of the Ruhr University Bochum center subgroup led by Tunn and colleagues was conducted 29 44 45 28 48 47 In this study the cyproterone acetate group was changed from intramuscular injections to 100 mg day oral cyproterone acetate 29 45 Of the 39 patients in the study the global 5 year survival rate was not significantly different between the estradiol undecylate and cyproterone acetate groups 24 and 26 respectively 29 45 28 48 47 In patients without metastases the 5 year survival rate was 51 in the cyproterone acetate group relative to 43 in the estradiol undecylate group although the difference was not statistically significant 29 45 In terms of non prostate cancer deaths there were 5 in the CPA group and 6 in the EU group 29 The incidence of cardiovascular related mortality was 3 deaths in the CPA group and 3 deaths in the EU group 29 vte Side effects of estradiol undecylate versus cyproterone acetate in men Side effect Estradiol undecylate100 mg month i m n 96 Cyproterone acetate100 mg day oral n 95 n n Gynecomastia 74 77 1 12 12 6 Breast tenderness 84 87 5 6 6 3 Sexual impotence Occurred in essentially all patients of both groups Leg edema 17 17 7 4 4 2 Thrombosis 4 4 2 5 5 3 Cardiovascular mortality 2 2 1 2 2 1 Other mortality 1a 1 0 0 0 Notes For 6 months in 191 men age 51 to 88 years with prostate cancer Footnotes Differences in incidences between groups were statistically significant a Due to unknown causes Sources See template The side effects of estradiol undecylate have also been studied and reported beyond the preceding clinical trial programme and for other patient populations for instance women Side effects during therapy with massive doses of estradiol undecylate 200 mg three times per week or 600 mg per week and around 2 400 mg per month total in postmenopausal women with advanced breast cancer have included appetite loss nausea vomiting vaginal bleeding vaginal discharge nipple pigmentation breast pain rash urinary incontinence edema drowsiness hypercalcemia and local injection site reactions 34 Like with other estrogens treatment with estradiol undecylate has been found to produce testicular abnormalities and disturbances of spermatogenesis in men 60 In transgender women estradiol undecylate by intramuscular injection at extremely high doses 200 800 mg month was associated with greater incidence of hyperprolactinemia high prolactin levels than ethinylestradiol orally at a dose of 100 mg day or about 3 mg month total rates of 40 and 16 for prolactin levels greater than 1 000 mU L respectively 35 Switching from estradiol undecylate to ethinylestradiol resulted in a decrease in prolactin levels in many individuals 35 The preceding dosage of estradiol undecylate corresponds to much greater estrogenic exposure than the dosage of ethinylestradiol 35 Cyproterone acetate was also used in combination with estrogen in the study 35 Overdose EditSee also Estradiol medication Overdose Estradiol undecylate has been used clinically at massive doses of as much as 800 to 2 400 mg per month by intramuscular injection given in divided doses of 100 to 200 mg per injection two to three times per week 34 15 35 36 37 For purposes of comparison a single 100 mg intramuscular injection of estradiol undecylate has been reported to produce estradiol levels of about 500 pg mL 61 Symptoms of estrogen overdosage may include nausea vomiting bloating increased weight water retention breast tenderness vaginal discharge heavy legs and leg cramps 39 These side effects can be diminished by reducing the estrogen dosage 39 Interactions EditSee also Estradiol medication Interactions Inhibitors and inducers of cytochrome P450 may influence the metabolism of estradiol and by extension circulating estradiol levels 62 Pharmacology Edit Estradiol the active form of estradiol undecylate Pharmacodynamics Edit See also Pharmacodynamics of estradiol Esters of estradiol like estradiol undecylate are readily hydrolyzed prodrugs of estradiol but have an extended duration when administered in oil via intramuscular injection due to a depot effect afforded by their fatty acid ester moiety 5 As prodrugs of estradiol estradiol undecylate and other estradiol esters are estrogens 4 5 Estradiol undecylate is of about 62 higher molecular weight than estradiol due to the presence of its C17b undecylate ester 9 11 Because estradiol undecylate is a prodrug of estradiol it is considered to be a natural and bioidentical form of estrogen 4 18 19 The effects of estradiol undecylate on cortisol dehydroepiandrosterone sulfate testosterone prolactin and sex hormone binding globulin levels as well as on the hypothalamic pituitary adrenal axis have been studied in men with prostate cancer and compared with those of high dose cyproterone acetate therapy 63 64 65 66 67 17 68 69 70 71 The effects of estradiol undecylate on serum lipids and ceruloplasmin levels have been studied as well 72 73 74 Additionally the influence of estradiol undecylate on SHBG levels and free testosterone fraction in women has been described 75 vte Potencies and durations of natural estrogens by intramuscular injection Estrogen Form Dose mg Duration by dose mg EPD CICDEstradiol Aq soln lt 1 dOil soln 40 60 1 2 1 2 dAq susp 3 5 0 5 2 2 7 d 3 5 gt 5 dMicrosph 1 30 dEstradiol benzoate Oil soln 25 35 1 66 2 3 d 5 3 6 dAq susp 20 10 16 21 dEmulsion 10 14 21 dEstradiol dipropionate Oil soln 25 30 5 5 8 dEstradiol valerate Oil soln 20 30 5 5 7 8 d 10 10 14 d 40 14 21 d 100 21 28 dEstradiol benz butyrate Oil soln 10 10 21 dEstradiol cypionate Oil soln 20 30 5 11 14 dAq susp 5 5 14 24 dEstradiol enanthate Oil soln 5 10 10 20 30 dEstradiol dienanthate Oil soln 7 5 gt 40 dEstradiol undecylate Oil soln 10 20 40 60 d 25 50 60 120 dPolyestradiol phosphate Aq soln 40 60 40 30 d 80 60 d 160 120 dEstrone Oil soln 1 2 2 3 dAq susp 0 1 2 2 7 dEstriol Oil soln 1 2 1 4 dPolyestriol phosphate Aq soln 50 30 d 80 60 dNotes and sourcesNotes All aqueous suspensions are of microcrystalline particle size Estradiol production during the menstrual cycle is 30 640 µg d 6 4 8 6 mg total per month or cycle The vaginal epithelium maturation dosage of estradiol benzoate or estradiol valerate has been reported as 5 to 7 mg week An effective ovulation inhibiting dose of estradiol undecylate is 20 30 mg month Sources See template Antigonadotropic activity Edit Testosterone levels with 300 mg week cyproterone acetate or 100 mg month estradiol undecylate both by intramuscular injection 17 The solid lines are the average levels and the dashed lines are the highest and lowest observed levels Estradiol testosterone and prolactin levels with 100 mg month estradiol undecylate by intramuscular injection in men with prostate cancer 65 A phase III clinical trial comparing high dose intramuscular cyproterone acetate 300 mg week and high dose intramuscular estradiol undecylate 100 mg month in the treatment of prostate cancer found that estradiol undecylate suppressed testosterone levels into the castrate range lt 50 ng dL 76 within at least 3 months whereas testosterone levels with cyproterone acetate were significantly higher and above the castrate range even after 6 months of treatment 17 With estradiol undecylate testosterone levels fell from 416 ng dL to 38 ng mL 91 after 3 months and to 29 6 ng dL 93 after 6 months whereas with cyproterone acetate testosterone levels fell from 434 ng dL to 107 ng mL 75 at 3 months and to 102 ng mL 76 at 6 months 17 In another study using the same dosages estradiol undecylate suppressed testosterone levels by 97 while CPA suppressed them by 70 67 In accordance whereas estrogens are well established as able to suppress testosterone levels into the castrate range at sufficiently high dosages 77 progestogens like cyproterone acetate on their own are able to decrease testosterone levels only up to an apparent maximum of around 70 to 80 78 79 Besides effects on testosterone levels the long term effects of estradiol undecylate on testicular morphology in transgender women have been studied 60 Pharmacokinetics Edit See also Pharmacokinetics of estradiol The pharmacokinetics of estradiol undecylate have been assessed limitedly in a few studies 80 81 82 83 65 84 7 8 Following a single intramuscular injection of 100 mg estradiol undecylate in oil mean levels of estradiol were about 500 pg mL a day after injection and about 340 pg mL 14 days after injection in 4 people 80 Levels of estradiol with intramuscular estradiol undecylate were reported to be very irregular and to vary by as much as 10 fold between individuals 80 In another study following a single intramuscular injection of 32 2 mg estradiol undecylate levels of estradiol peaked at around 400 pg mL after 3 days and decreased from this peak to around 200 pg mL after 6 days in 3 postmenopausal women 81 85 In a repeated administration study of 100 mg per month estradiol undecylate in 14 men with prostate cancer estradiol levels at trough were about 560 pg mL at 3 months and about 540 pg mL at 6 months following initiation of therapy 65 In a larger follow up of the study with 21 men estradiol levels at trough were about 36 pg mL at baseline 486 pg mL at 3 months and 598 pg mL at 6 months of therapy 70 In one further study levels of estradiol in an unspecified number of postmenopausal women following a single injection of 100 mg estradiol undecylate were said to be between 300 pg mL and 600 pg mL six days post injection 75 Due to its more protracted duration doses of estradiol undecylate that are typical of other estradiol esters produce only subthreshold estradiol levels and for this reason higher single doses of estradiol undecylate are necessary for similar effects 86 80 81 However the relatively low levels of estradiol produced by lower doses of estradiol undecylate are favorable for menopausal replacement therapy 86 The duration of estradiol undecylate is markedly prolonged relative to that of estradiol benzoate estradiol valerate and many other estradiol esters 61 6 20 18 A single intramuscular injection of 10 to 12 5 mg estradiol undecylate has a duration of 40 to 60 days 1 2 months and of 25 to 50 mg estradiol undecylate has an estimated duration of effect of 2 to 4 months in postmenopausal women 7 8 6 20 A single intramuscular injection of 20 to 30 mg estradiol undecylate has been found to inhibit ovulation when used as an estrogen only injectable contraceptive in premenopausal women for 1 to 3 months mean 1 7 months as well 87 When used at a higher dose of 100 mg per injection in men with prostate cancer estradiol undecylate has been given usually once a month 17 32 After a single subcutaneous injection of estradiol undecylate in rats its duration of effect was 80 days about 2 5 months 88 89 90 Due to its very prolonged duration estradiol undecylate has been described in general as a favorable alternative to estradiol implants 8 The excretion of estradiol undecylate has been studied as well 83 Estradiol undecylate has not been used via oral administration However a closely related estradiol ester estradiol decanoate estradiol decylate has been studied via the oral route and has been found to possess significant oral bioavailability to produce relatively high estradiol levels of about 100 pg mL after a single 0 5 mg oral dose and about 100 to 150 pg mL with continuous 0 25 mg day oral therapy and to have a much higher estradiol to estrone ratio than oral estradiol of about 2 1 91 92 93 It is thought that this is due to absorption of estradiol decanoate by the lymphatic system and a consequent partial bypass of first pass metabolism in the liver and intestines 91 92 93 which is similarly known to occur with oral testosterone undecanoate 94 95 Hormone levels with estradiol undecylate by intramuscular injection Estradiol levels after a single intramuscular injection of 10 mg estradiol valerate in oil or 100 mg estradiol undecylate in oil both in 4 individuals each 61 Subject characteristics and assay method were not described 61 Source was Vermeulen 1975 61 Estradiol levels after a short intravenous infusion of 20 mg estradiol in aqueous solution or an intramuscular injection of equimolar doses of estradiol esters in oil solution in 3 postmenopausal women each 82 96 Assays were performed using radioimmunoassay with chromatographic separation 82 96 Sources were Geppert 1975 and Leyendecker et al 1975 82 96 Estradiol testosterone luteinizing hormone and follicle stimulating hormone levels with an intramuscular injection of 32 3 mg estradiol undecylate in oil in 3 postmenopausal women 82 96 Assays were performed using radioimmunoassay with chromatographic separation 96 82 Sources were Geppert 1975 and Leyendecker et al 1975 82 96 Estradiol testosterone and prolactin levels with 100 mg month estradiol undecylate in oil by intramuscular injection in 14 to 28 men with prostate cancer 65 A follow up of the study with more men and with additional hormones was also subsequently published 70 Sources were Jacobi amp Altwein 1979 and Derra 1981 65 70 Chemistry EditSee also Estrogen ester and List of estrogen esters Estradiol esters Estradiol undecylate is a synthetic estrane steroid and an estradiol ester 9 10 It is specifically the C17b undecylate undecanoate ester of estradiol 9 10 11 The compound is also known as estradiol 17b undecylate or as estra 1 3 5 10 triene 3 17b diol 17b undecanoate 10 11 The undecylic acid undecanoic acid ester of estradiol undecylate is a medium chain fatty acid and is found naturally in many foods some examples of which include coconut fruits fats oils and rice 97 Estradiol undecylate is a relatively long chain ester of estradiol 10 11 Its undecylate ester contains 11 carbon atoms 10 11 For comparison the ester chains of estradiol acetate estradiol valerate and estradiol enantate have 2 5 and 7 carbon atoms respectively 10 11 As a result of its longer ester chain estradiol undecylate is the most lipophilic of these estradiol esters and for this reason has by far the longest duration when administered in oil solution by intramuscular injection 61 98 99 An example of an estradiol ester with a longer ester chain than estradiol undecylate is estradiol stearate Depofollan which has 18 carbon atoms and has been used in medicine as an estrogen as well A few estradiol esters related to estradiol undecylate include estradiol decanoate estradiol diundecylate and estradiol diundecylenate 9 10 Estradiol undecylate shares the same undecylate ester as testosterone undecanoate an androgen anabolic steroid and very long lasting testosterone ester 9 10 Estradiol undecylate is one of the longest chain steroid esters that has been in common medical use 100 vte Structural properties of selected estradiol esters Estrogen Structure Ester s Relativemol weight RelativeE2 contentb log PcPosition s Moiet ies Type LengthaEstradiol 1 00 1 00 4 0Estradiol acetate C3 Ethanoic acid Straight chain fatty acid 2 1 15 0 87 4 2Estradiol benzoate C3 Benzenecarboxylic acid Aromatic fatty acid 4 5 1 38 0 72 4 7Estradiol dipropionate C3 C17b Propanoic acid 2 Straight chain fatty acid 3 2 1 41 0 71 4 9Estradiol valerate C17b Pentanoic acid Straight chain fatty acid 5 1 31 0 76 5 6 6 3Estradiol benzoate butyrate C3 C17b Benzoic acid butyric acid Mixed fatty acid 6 2 1 64 0 61 6 3Estradiol cypionate C17b Cyclopentylpropanoic acid Aromatic fatty acid 6 1 46 0 69 6 9Estradiol enanthate C17b Heptanoic acid Straight chain fatty acid 7 1 41 0 71 6 7 7 3Estradiol dienanthate C3 C17b Heptanoic acid 2 Straight chain fatty acid 7 2 1 82 0 55 8 1 10 4Estradiol undecylate C17b Undecanoic acid Straight chain fatty acid 11 1 62 0 62 9 2 9 8Estradiol stearate C17b Octadecanoic acid Straight chain fatty acid 18 1 98 0 51 12 2 12 4Estradiol distearate C3 C17b Octadecanoic acid 2 Straight chain fatty acid 18 2 2 96 0 34 20 2Estradiol sulfate C3 Sulfuric acid Water soluble conjugate 1 29 0 77 0 3 3 8Estradiol glucuronide C17b Glucuronic acid Water soluble conjugate 1 65 0 61 2 1 2 7Estramustine phosphated C3 C17b Normustine phosphoric acid Water soluble conjugate 1 91 0 52 2 9 5 0Polyestradiol phosphatee C3 C17b Phosphoric acid Water soluble conjugate 1 23f 0 81f 2 9gFootnotes a Length of ester in carbon atoms for straight chain fatty acids or approximate length of ester in carbon atoms for aromatic fatty acids b Relative estradiol content by weight i e relative estrogenic exposure c Experimental or predicted octanol water partition coefficient i e lipophilicity hydrophobicity Retrieved from PubChem ChemSpider and DrugBank d Also known as estradiol normustine phosphate e Polymer of estradiol phosphate 13 repeat units f Relative molecular weight or estradiol content per repeat unit g log P of repeat unit i e estradiol phosphate Sources See individual articles History EditEstradiol undecylate was first described in the scientific literature along with estradiol valerate and a variety of other estradiol esters by Karl Junkmann of Schering AG in 1953 101 7 It was introduced for medical use via intramuscular injection by 1956 21 8 22 Syntex applied for a patent for estradiol undecylate in 1958 which was granted in 1961 and was given a priority date of 1957 23 102 Estradiol undecylate was introduced for medical use and was employed for decades but was eventually discontinued 11 25 38 It remained in use in some countries as late as the 2000s 23 11 24 Harry Benjamin reported on the use of estradiol undecylate in transgender women in his book The Transsexual Phenomenon in 1966 and in a literature review in the Journal of Sex Research in 1967 14 103 Society and culture EditGeneric names Edit Estradiol undecylate is the generic name of the drug and its INN and USAN 9 10 11 16 It is also spelled in some publications as estradiol unducelate and is also known as estradiol undecanoate 61 9 10 11 16 In German it is known under a variety of spellings including as estradiolundecylat ostradiolundecylat ostradiolundezylat oestradiolundecylat oestradiolundezylat and others 104 Estradiol undecylate is known by its former developmental code names RS 1047 and SQ 9993 as well 9 10 11 16 Brand names Edit The major brand name of estradiol undecylate is Progynon Depot 100 9 10 11 It has also been marketed under other brand names including Delestrec Depogin Estrolent Oestradiol D Oestradiol Retard Theramex and Primogyn Depot 0 1 mg ml among others 9 10 11 23 24 Availability Edit Estradiol undecylate was available in the Europe including in France Germany Great Britain Monaco the Netherlands Switzerland and Japan 11 23 105 22 106 However it has been discontinued and hence is no longer available 25 38 Research EditEstradiol undecylate was studied by Schering alone as an estrogen only injectable contraceptive in premenopausal women at a dose of 20 to 30 mg once a month 85 87 107 108 It was effective lacked breast and thromboembolic complications lacked other side effects besides amenorrhea and prevented ovulation for 1 to 3 months mean 1 7 months following a single dose 87 However uterine growth of 1 to 2 cm was observed after one year and endometrial hyperplasia was occasionally encountered 85 87 107 The preparation was not further developed as a form of birth control due to the risks of endometrial hyperplasia and cancer associated with long term unopposed estrogen therapy 87 Estradiol undecylate in combination with norethisterone enanthate at doses of 5 to 10 mg and 50 to 70 mg respectively was studied by Schering as a combined injectable contraceptive in premenopausal women and was found to be effective and well tolerated but ultimately was not marketed for this use 109 108 87 110 111 112 See also EditEstradiol undecylate norethisterone enanthateReferences Edit a b c d Zink C 1 January 1988 Dictionary of Obstetrics and Gynecology Walter de Gruyter p 85 ISBN 978 3 11 085727 6 Stanczyk FZ Archer DF Bhavnani BR June 2013 Ethinyl estradiol and 17b estradiol in combined oral contraceptives pharmacokinetics pharmacodynamics and risk assessment Contraception 87 6 706 727 doi 10 1016 j contraception 2012 12 011 PMID 23375353 Falcone T Hurd WW 2007 Clinical Reproductive Medicine and Surgery Elsevier Health Sciences pp 22 362 388 ISBN 978 0 323 03309 1 a b c d e f g Oettel M Schillinger E 6 December 2012 Estrogens and Antiestrogens II Pharmacology and Clinical Application of Estrogens and Antiestrogen Springer Science amp Business Media p 261 544 ISBN 978 3 642 60107 1 Natural estrogens considered here include Esters of 17b estradiol such as estradiol valerate estradiol benzoate and estradiol cypionate Esterification aims at either better absorption after oral administration or a sustained release from the depot after intramuscular administration During absorption the esters are cleaved by endogenous esterases and the pharmacologically active 17b estradiol is released therefore the esters are considered as natural estrogens a b c d e f Kuhl H August 2005 Pharmacology of estrogens and progestogens influence of different routes of administration Climacteric 8 Suppl 1 3 63 doi 10 1080 13697130500148875 PMID 16112947 S2CID 24616324 a b c d Labhart A 6 December 2012 Clinical Endocrinology Theory and Practice Springer Science amp Business Media pp 551 553 ISBN 978 3 642 96158 8 a b c d e f Wied GL January 1954 Estradiol valerate and estradiol undecylate two new estrogens with prolonged action comparison with estradiol benzoate Estradiol valerate and estradiol undecylate two new estrogens with prolonged action comparison with estradiol benzoate Geburtshilfe und Frauenheilkunde in German 14 1 45 52 PMID 13142295 a b c d e f g h Gouygou C Gueritee N Pye A 1956 A fat soluble delayed estrogen the estradiol undecylate A fat soluble delayed estrogen the estradiol undecylate Therapie in French 11 5 909 917 PMID 13391788 a b c d e f g h i j k Elks J 14 November 2014 The Dictionary of Drugs Chemical Data Chemical Data Structures and Bibliographies Springer pp 898 ISBN 978 1 4757 2085 3 a b c d e f g h i j k l m n Roberts AD 1991 Dictionary of Steroids Chemical Data Structures and Bibliographies CRC Press p 415 ISBN 978 0 412 27060 4 Retrieved 20 May 2012 a b c d e f g h i j k l m n o p q r Index Nominum 2000 International Drug Directory Taylor amp Francis US 2000 p 405 ISBN 978 3 88763 075 1 Retrieved 20 May 2012 a b c d e f Norman G Dean ME Langley RE Hodges ZC Ritchie G Parmar MK et al February 2008 Parenteral oestrogen in the treatment of prostate cancer a systematic review British Journal of Cancer 98 4 697 707 doi 10 1038 sj bjc 6604230 PMC 2259178 PMID 18268497 a b c Schlatterer K von Werder K Stalla GK 1996 Multistep treatment concept of transsexual patients Experimental and Clinical Endocrinology amp Diabetes 104 6 413 419 doi 10 1055 s 0029 1211479 PMID 9021341 a b c d e Benjamin H Lal GB Green R Masters RE 1966 The Transsexual Phenomenon Ace Publishing Company p 107 Another preparation of even higher potency is Squibb s Delestrec which at this writing is not yet on the market in the United States but is well known in Germany and other European countries under the name of Progynon Depot Schering It is chemically Estradiol Undecylate in oil likewise slowly absorbing and containing 100 mg to 1 cc Injections of 1 cc once or twice a month can be sufficient Occasionally however larger doses are required to influence the patient s emotional distress a b c d Israel GE March 2001 Transgender Care Recommended Guidelines Practical Information and Personal Accounts Temple University Press pp 64 ISBN 978 1 56639 852 7 a b c d Estradiol a b c d e f g h i j k l m n o Jacobi GH Altwein JE Kurth KH Basting R Hohenfellner R June 1980 Treatment of advanced prostatic cancer with parenteral cyproterone acetate a phase III randomised trial British Journal of Urology 52 3 208 215 doi 10 1111 j 1464 410x 1980 tb02961 x PMID 7000222 a b c International Society of Urology 1973 Reports of the Congress Livingstone p 252 Progynon Depot ist eine Oestrogenpraparat mit einem Depoteffekt von 4 6 Wochen 1 ml Progynon Depot 100 mg enthalt 100 mg Oestra diolundecylat in oliger Losung Oestradiolundecylat ist ein Ester des naturlichen Oestrogens Oestradiol a b Lembeck F Sewing KF 7 March 2013 Pharmakologie Fibel Tafeln zur Pharmakologie Vorlesung Springer Verlag pp 113 ISBN 978 3 642 65621 7 a b c Wilde PR Coombs CF Short AJ 1959 The Medical Annual A Year Book of Treatment and Practitioner s Index Publishing Science Group As in the case of progestogens the esters of oestradiol vary in the duration of their effect Oestradiol benzoate is short acting three days to a week Oestradiol valerianate is somewhat longer acting and oestradiol enanthate and undecylate have considerably more prolonged duration of effectiveness The undecylate may remain effective for some months and should not be employed a b Halkerston ID Hillman J Palmer D Rundle A July 1956 Changes in the excretion pattern of neutral 17 ketosteroids during oestrogen administration to male subjects The Journal of Endocrinology 13 4 433 438 doi 10 1677 joe 0 0130433 PMID 13345960 a b c Bishop PM 1958 Endocrine Treatment of Gynaecological Disorders In Gardiner Hill H ed Modern Trends in Endocrinology Modern Trends Vol 1 London Butterworth amp Co pp 231 244 a b c d e f Kleemann A Engel J Kutscher B Reichert D 2009 Pharmaceutical Substances Syntheses Patents and Applications of the most relevant APIs 5th ed Thieme pp 1167 1174 ISBN 978 3 13 179525 0 a b c Index Nominum International Drug Directory CRC Press 2004 pp 469 ISBN 978 3 88763 101 7 a b c Micromedex Mutschler E Derendorf H 1995 Drug Actions Basic Principles and Therapeutic Aspects CRC Press p 609 ISBN 978 0 8493 7774 7 Retrieved 30 January 2013 Enfedjieff M March 1974 Experiences with hormonal treatment of prostatic carcinoma Experiences with hormonal treatment of prostatic carcinoma Zeitschrift fur Urologie und Nephrologie in German 67 3 171 173 PMID 4848715 Archived from the original on 2018 11 23 Treatment of prostatic carcinoma in 256 patients using parenteral injections of Progynon Depot a depto estradiol preparation is reproted 58 of patients survived 3 or more years from beginning of treatment and in 70 therapeutic results were considered good with regression of tumor mass reduction or disappearance of pain normalization of miction and improved general status Results of estrogen treatment are evident within 3 months in most cases Side effects include gynecomastia in 95 of cases impotence in almost all patients and atrophic changes in the testicles which may actually be desirable Prostatectomy is not recommended because of the high incidence of metastases even when prostatic disease is still small because of the high operative mortality and because of the undesirable after effects Orchidectomy was performed in patients in whom the prostatic capsule had been invaded or who had distant metastases Estrogen therapy for prostatic carcinoma gives excellent results and is very easy for both patient and physician a b c d e f g Tunn UW 1987 Antiandrogene in der Therapie des fortgeschrittenen Prostatakarzinoms Antiandrogens in the Treatment of Advanced Prostate Cancer Konservative Therapie des Prostatakarzinoms Conservative Therapy of Prostate Cancer in German pp 113 121 doi 10 1007 978 3 642 72613 2 12 ISBN 978 3 540 17724 1 a b c d e f g Saborowski KJ 1988 Konservative Therapie mit Cyproteronacetat und Estradiolundecylat beim Fortgeschrittenen Prostatacarcinom Eine 5 Jahres Studie Conservative Therapy with Cyproterone Acetate and Estradiol Undecylate in Advanced Prostate Cancer A 5 Year Study in German Bochum Univ Diss OCLC 917571781 OL 24895092W Mollard P March 1963 Clinical action of estradiol undecylate in the treatment of prostatic cancer Clinical action of estradiol undecylate in the treatment of prostatic cancer Lyon Medical in French 209 759 765 PMID 13935867 Schubert GE Ziegler H Volter D 1973 Comparison of histological and cytological studies of the prostate with special reference to oestrogene induced changes author s transl Comparison of histological and cytological studies of the prostate with special reference to oestrogene induced changes Verhandlungen der Deutschen Gesellschaft fur Pathologie in German 57 315 318 PMID 4142204 Archived from the original on 2018 11 23 Retrieved 2018 11 23 a b Satoskar RS Bhandarkar SD Rege NN 1973 Pharmacology and Pharmacotherapeutics Popular Prakashan pp 934 ISBN 978 81 7991 527 1 a b Morgan HG Morgan MH 1984 Aids to Psychiatry Churchill Livingstone p 75 ISBN 978 0 443 02613 3 Treatment of sexual offenders Hormone therapy Oestrogens may cause breast hypertrophy testicular atrophy osteoporosis oral ethinyl oestradiol 0 01 0 05 mg day causes least nausea Depot preparation oestradiol undecyleate 50 100mg once every 3 4 weeks Benperidol or butyrophenone and the antiandrogen cyproterone acetate also used a b c Kennedy BJ April 1967 Effect of massive doses of estradiol undecylate in advanced breast cancer Cancer Chemother Rep 51 2 491 495 a b c d e f Asscheman H Gooren LJ Assies J Smits JP de Slegte R June 1988 Prolactin levels and pituitary enlargement in hormone treated male to female transsexuals Clinical Endocrinology 28 6 583 588 doi 10 1111 j 1365 2265 1988 tb03849 x PMID 2978262 S2CID 29214187 a b Asscheman H Gooren LJ Eklund PL September 1989 Mortality and morbidity in transsexual patients with cross gender hormone treatment Metabolism 38 9 869 873 doi 10 1016 0026 0495 89 90233 3 PMID 2528051 a b Gazzeri R Galarza M Gazzeri G December 2007 Growth of a meningioma in a transsexual patient after estrogen progestin therapy The New England Journal of Medicine 357 23 2411 2412 doi 10 1056 NEJMc071938 PMID 18057351 a b c Sweetman SC ed 2009 Sex hormones and their modulators Martindale The Complete Drug Reference 36th ed London Pharmaceutical Press p 2098 ISBN 978 0 85369 840 1 a b c Lauritzen C September 1990 Clinical use of oestrogens and progestogens Maturitas 12 3 199 214 doi 10 1016 0378 5122 90 90004 P PMID 2215269 Lauritzen C Studd JW 22 June 2005 Current Management of the Menopause CRC Press pp 95 98 488 ISBN 978 0 203 48612 2 Laurtizen C 2001 Hormone Substitution Before During and After Menopause PDF In Fisch FH ed Menopause Andropause Hormone Replacement Therapy Through the Ages Krause amp Pachernegg Gablitz pp 67 88 ISBN 978 3 901299 34 6 Midwinter A 1976 Contraindications to estrogen therapy and management of the menopausal syndrome in these cases In Campbell S ed The Management of the Menopause amp Post Menopausal Years The Proceedings of the International Symposium held in London 24 26 November 1975 Arranged by the Institute of Obstetrics and Gynaecology The University of London MTP Press Limited pp 377 382 doi 10 1007 978 94 011 6165 7 33 ISBN 978 94 011 6167 1 a b c d e f g h i j k Jacobi GH June 1982 Intramuscular cyproterone acetate treatment for advanced prostatic carcinoma results of the first multicentric randomized trial In Schroder FH ed Proceedings Androgens and Anti androgens International Symposium Utrecht June 5th 1982 Schering Nederland BV pp 161 169 ISBN 978 9090004327 OCLC 11786945 a b Tunn UW Graff J Senge T June 1982 Treatment of inoperable prostatic cancer with cyproterone acetate In Schroder FH ed Proceedings Androgens and Anti androgens International Symposium Utrecht June 5th 1982 Schering Nederland BV pp 149 159 ISBN 978 9090004327 OCLC 11786945 a b c d e f g h i j Tunn UW Radlmaier A Neumann F 1988 Antiandrogens in Cancer Treatment In Stoll BA ed Endocrine Management of Cancer Contemporary Therapy pp 43 56 doi 10 1159 000415355 ISBN 978 3 8055 4686 7 a b c d e f g Schroder FH Radlmaier A 2009 Steroidal Antiandrogens In Jordan VC Furr BJ eds Hormone Therapy in Breast and Prostate Cancer Humana Press pp 325 346 doi 10 1007 978 1 59259 152 7 15 ISBN 978 1 60761 471 5 a b c d e f Ackermann R Altwein JE Faul P 13 March 2013 Aktuelle Therapie des Prostatakarzinoms Springer Verlag pp 276 277 ISBN 978 3 642 84264 1 a b c d Namer M October 1988 Clinical applications of antiandrogens Journal of Steroid Biochemistry 31 4B 719 729 doi 10 1016 0022 4731 88 90023 4 PMID 2462132 a b c d e Jacobi GR Tunn UW Senge TH 1 December 1982 Clinical experience with cyproterone acetate for palliation of inoperable prostate cancer In Jacobi GH Hohenfellner R eds Prostate Cancer Williams amp Wilkins pp 305 319 ISBN 978 0 683 04354 9 Altwein JE Jacobi GH Hohenfellner R 1978 Estrogen versus cyproterone acetate in untreated inoperable carcinoma of the prostate first results of an open prospective randomized study Abstracts 3rd Congress of the European Association of Urology Monte Carlo a b c d e Saygin D Tabib T Bittar HE Valenzi E Sembrat J Chan SY et al 1983 Transcriptional profiling of lung cell populations in idiopathic pulmonary arterial hypertension Pulmonary Circulation 10 1 40 48 doi 10 1007 BF00326861 PMC 7052475 PMID 32166015 S2CID 23447326 Jacobi GH Wenderoth UK 1982 Gonadotropin releasing hormone analogues for prostate cancer untoward side effects of high dose regimens acquire a therapeutical dimension European Urology 8 3 129 134 doi 10 1159 000473499 PMID 6281023 Ockrim J Lalani EN Abel P October 2006 Therapy Insight parenteral estrogen treatment for prostate cancer a new dawn for an old therapy Nature Clinical Practice Oncology 3 10 552 563 doi 10 1038 ncponc0602 PMID 17019433 S2CID 6847203 Lycette JL Bland LB Garzotto M Beer TM December 2006 Parenteral estrogens for prostate cancer can a new route of administration overcome old toxicities Clinical Genitourinary Cancer 5 3 198 205 doi 10 3816 CGC 2006 n 037 PMID 17239273 Russell N Cheung A Grossmann M August 2017 Estradiol for the mitigation of adverse effects of androgen deprivation therapy Endocrine Related Cancer 24 8 R297 R313 doi 10 1530 ERC 17 0153 PMID 28667081 Langley RE Cafferty FH Alhasso AA Rosen SD Sundaram SK Freeman SC et al April 2013 Cardiovascular outcomes in patients with locally advanced and metastatic prostate cancer treated with luteinising hormone releasing hormone agonists or transdermal oestrogen the randomised phase 2 MRC PATCH trial PR09 The Lancet Oncology 14 4 306 316 doi 10 1016 S1470 2045 13 70025 1 PMC 3620898 PMID 23465742 Langley RE Gilbert DC Duong T Clarke NW Nankivell M Rosen SD et al February 2021 Transdermal oestradiol for androgen suppression in prostate cancer long term cardiovascular outcomes from the randomised Prostate Adenocarcinoma Transcutaneous Hormone PATCH trial programme PDF Lancet 397 10274 581 591 doi 10 1016 S0140 6736 21 00100 8 PMC 7614681 PMID 33581820 S2CID 231885186 Tunn UW Senge T Jacobi GH 1983 Erfahrungen mit Cyproteronacetat als Monotherapie beim Inoperablen Prostatakarzinom Experience with Cyproterone Acetate as Monotherapy for Inoperable Prostate Cancer In Klosterhalfen H ed Therapie des Fortgeschrittenen Prostatakarzinoms Vortragsveranstaltung fur Urologen Berlin 1982 83 Therapy of Advanced Prostate Cancer Lecture Event for Urologists Berlin 1982 83 Wiss Buchreihe Schering AG pp 67 76 ISBN 978 3921817162 OCLC 67592679 Schroder FH 1996 Cyproterone Acetate Results of Clinical Trials and Indications for Use in Human Prostate Cancer Antiandrogens in Prostate Cancer pp 45 51 doi 10 1007 978 3 642 45745 6 4 ISBN 978 3 642 45747 0 a b Schulze C January 1988 Response of the human testis to long term estrogen treatment morphology of Sertoli cells Leydig cells and spermatogonial stem cells Cell and Tissue Research 251 1 31 43 doi 10 1007 BF00215444 PMID 3342442 S2CID 22847105 a b c d e f g Vermeulen A 1975 Longacting steroid preparations Acta Clinica Belgica 30 1 48 55 doi 10 1080 17843286 1975 11716973 PMID 1231448 Cheng ZN Shu Y Liu ZQ Wang LS Ou Yang DS Zhou HH February 2001 Role of cytochrome P450 in estradiol metabolism in vitro Acta Pharmacologica Sinica 22 2 148 154 PMID 11741520 Schurmeyer T Graff J Senge T Nieschlag E March 1986 Effect of oestrogen or cyproterone acetate treatment on adrenocortical function in prostate carcinoma patients Acta Endocrinologica 111 3 360 367 doi 10 1530 acta 0 1110360 PMID 2421511 Spona J Lunglmayr G July 1980 Prolaktin Serumspiegel unter Behandlung des Prostatakarzinoms mit Ostradiol 17 beta undezylat und Cyproteronazetat Verhandlungsbericht der Deutschen Gesellschaft fur Urologie Serum Prolactin Levels During Therapy of Prostatic Cancer with Estradiol 17 beta undecylate and Cyproterone Acetate pp 494 7 doi 10 1007 978 3 642 81706 9 120 ISBN 978 3 540 11017 0 PMID 6933738 a href Template Cite book html title Template Cite book cite book a journal ignored help a b c d e f Jacobi GH Altwein JE 1979 Bromocriptin als Palliativtherapie beim fortgeschrittenen Prostatakarzinom Experimentelles und klinisches Profil eines Medikamentes Bromocriptine as Palliative Therapy in Advanced Prostate Cancer Experimental and Clinical Profile of a Drug Urologia Internationalis 34 4 266 290 doi 10 1159 000280272 PMID 89747 Schulze H Senge T 1987 Konservative Therapie des Prostatakarzinoms pp 89 98 doi 10 1007 978 3 642 72613 2 8 ISBN 978 3 540 17724 1 a b Neumann F El Etreby MF Habenicht U Radlmaier A Bormacher K 1987 Options for androgen withdrawal and total blockage pp 61 86 doi 10 1007 978 3 642 72613 2 6 ISBN 978 3 540 17724 1 Tunn UW Senge T Neumann F 1981 Serumkonzentrationen von Testosteron und Prolaktin nach operativer und medikamentoser Kastration eine Langzeitstudie bei Prostatakarzinom Patienten Verhandlungsbericht der Deutschen Gesellschaft fur Urologie Serum concentrations of testosterone and prolactin after surgical and medical castration A long term study in prostate cancer patients Vol 32 pp 419 421 doi 10 1007 978 3 642 81706 9 123 ISBN 978 3 540 11017 0 Baba S Janetschek G Wenderoth U Jacobi GH 1981 Beeinflussung des intraprostatischen Testosteron Stoffwechsels durch Cyproteronazetat und Ostradiolundecylat bei Patienten mit Prostatakarzinom In vivo Untersuchungen Verhandlungsbericht der Deutschen Gesellschaft fur Urologie Influence of intraprostatic testosterone metabolism by cyproterone acetate and estradiol undecylate in patients with prostate cancer in vivo studies Vol 32 pp 464 466 doi 10 1007 978 3 642 81706 9 138 ISBN 978 3 540 11017 0 a b c d Derra C 1981 Hormonprofile unter Ostrogen und Antiandrogentherapie bei Patienten mit Prostatakarzinom Ostradiolundecylat versus Cyproteronacetat Hormone profiles under estrogen and antiandrogen therapy in patients with prostate cancer estradiol undecylate versus cyproterone acetate Ph D thesis Mainz Universiẗat OCLC 65055508 OL 24894194W Jacobi GH Altwein JE 1980 Testosterone plasma kinetics in patients with prostatic carcinoma treated with estradiol undecylate cyproterone acetate and estramustine phosphate a preliminary report Steroid receptors metabolism and prostatic cancer proceedings of a workshop of the Society of Urologic Oncology and Endocrinology Amsterdam 27 28 April 1979 Vol 494 Excerpta Medica pp 144 151 Nagel R Schillinger E Kolln CP Pochhammer K 1973 24 Tagung vom 13 Bis 16 September 1972 in Hannover The behavior of serum lipids in patients with prostate cancer after treatment with estradiol undecylate Verhandlungsbericht der Deutschen Gesellschaft fur Urologie Vol 24 pp 298 301 doi 10 1007 978 3 642 80738 1 75 ISBN 978 3 540 06186 1 Taupitz A Otaguro K 1959 Quantitative Examination of Serum Components After Antiandrogenic Therapy Against Prostatic Cancer Quantitative Examination of Serum Components after Antiandrogenic Therapy Against Prostatic Cancer Clinical and Experimental Observation The Japanese Journal of Urology 50 3 153 162 doi 10 5980 jpnjurol1928 50 3 153 Gotz H Ehrmeier H June 1971 Estrogens and ceruloplasmine level Estrogens and ceruloplasmin levels Archiv fur Gynakologie 211 1 204 206 doi 10 1007 BF00682878 PMID 5108847 S2CID 38378905 a b Vermeulen A 1977 Transport and distribution of androgens at different ages In Martini L Motta M eds Androgens and Antiandrogens New York Raven Press pp 53 65 ISBN 9780890041413 OCLC 925036459 In postmenopausal women however estrogen administration does not change the androgen levels significantly The increase in TeBG capacity after injection of 100 mg Progynon Depot estradiol undecylate therefore is unequivocally the result of the estrogens 6 days after injection when plasma estradiol levels varied between 30 ng 100 ml 300 pg mL and 60 ng 100 ml 600 pg mL TeBG levels were nearly doubled 1 4 1 6 107 M whereas the free testosterone fraction decreased from 1 25 to 0 70 Saleh FM 11 February 2009 Sex Offenders Identification Risk Assessment Treatment and Legal Issues Oxford University Press USA pp 176 ISBN 978 0 19 517704 6 Salam MA 2003 Principles amp Practice of Urology A Comprehensive Text Universal Publishers pp 684 ISBN 978 1 58112 412 5 Wein AJ Kavoussi LR Novick AC Partin AW Peters CA 25 August 2011 Campbell Walsh Urology Expert Consult Premium Edition Enhanced Online Features and Print 4 Volume Set Elsevier Health Sciences pp 2938 ISBN 978 1 4160 6911 9 Kjeld JM Puah CM Kaufman B Loizou S Vlotides J Gwee HM et al November 1979 Effects of norgestrel and ethinyloestradiol ingestion on serum levels of sex hormones and gonadotrophins in men Clinical Endocrinology 11 5 497 504 doi 10 1111 j 1365 2265 1979 tb03102 x PMID 519881 S2CID 5836155 a b c d Vermeulen A 1975 Longacting steroid preparations Acta Clinica Belgica 30 1 48 55 doi 10 1080 17843286 1975 11716973 PMID 1231448 a b c Leyendecker G Geppert G Nocke W Ufer J May 1975 Estradiol 17beta estrone LH and FSH in serum after administration of estradiol 17beta estradiolbenzoate estradiol valeriate and estradiol undecylate in the female author s transl Estradiol 17b estrone LH and FSH in serum after administration of estradiol 17b estradiol benzoate estradiol valeriate and estradiol undecylate in the female Geburtshilfe und Frauenheilkunde in German 35 5 370 374 PMID 1150068 Estradiol 17b estradiol benzoate estradiol valerianate and estradiol undecylate were injected intravenously and intramuscularly to postmenopausal woman and to female castrates Equal doses were used corresponding to 20 mg of free estradiol 17b Estradiol 17b estrone FSH and LH were measured in serum by radioimmunoassay before and after application of the hormone and the estradiol esters Thus the depot effect of the different esters could be compared a b c d e f g Geppert G 1975 Untersuchungen zur Pharmakokinetik von Ostradiol 17b Ostradiol Benzoat Ostradiol Valerianat und Ostradiol Undezylat bei der Frau der Verlauf der Konzentrationen von Ostradiol 17b Ostron LH und FSH im Serum Studies on the pharmacokinetics of estradiol 17b estradiol benzoate estradiol valerate and estradiol undecylate in women the progression of serum estradiol 17b estrone LH and FSH concentrations pp 1 34 OCLC 632312599 a b Zimmermann W Buescher HK Taupitz A Thewalt K 1964 Steroidhormonausscheidung bei Patienten mit Erkrankungen der Prostata Unter Behandlung mit Naturlichen und Synthetischen Oestrogenen Steroid Hormone Excretion of Patients with Diseases of the Prostate under Treatment with Natural and Synthetic Estrogens Acta Endocrinologica in German 45 4 Suppl 90 SUPPL90 211 SUPPL90 225 doi 10 1530 acta 0 045S211 PMID 14111328 Oriowo MA Landgren BM Stenstrom B Diczfalusy E April 1980 A comparison of the pharmacokinetic properties of three estradiol esters Contraception 21 4 415 424 doi 10 1016 S0010 7824 80 80018 7 PMID 7389356 a b c Brotherton J 1976 Sex Hormone Pharmacology Academic Press pp 226 476 ISBN 978 0 12 137250 7 a b Jucker E 8 March 2013 Fortschritte der Arzneimittelforschung Progress in Drug Research Progres des recherches pharmaceutiques Birkhauser pp 243 ISBN 978 3 0348 7044 3 Estradiol undecylenate has a more protracted effect but it releases only subthreshold doses of steroid advantage may be taken of this for the treatment of menopause a b c d e f Toppozada M June 1977 The clinical use of monthly injectable contraceptive preparations Obstetrical amp Gynecological Survey 32 6 335 347 doi 10 1097 00006254 197706000 00001 PMID 865726 Kuhl H Taubert HD July 1973 A new class of long acting hormonal steroid preparation synthesis of oligomeric estradiol derivatives Steroids 22 1 73 87 doi 10 1016 0039 128X 73 90072 X PMID 4737545 Kuhl H Taubert HD September 1973 Proceedings New type of long acting steroids Synthesis and biological effect A New Type of Long Acting Steroid Preparation Synthesis and Biological Efficacy Archiv fur Gynakologie 214 1 127 128 doi 10 1007 BF00671087 PMID 4801412 S2CID 26261148 Kuhl H Auerhammer W Taubert HD October 1976 Oligomeric oestradiol esters a new class of long acting oestrogens Acta Endocrinologica 83 2 439 448 doi 10 1530 acta 0 0830439 PMID 989671 a b Kicovic PM Luisi M Franchi F Alicicco E July 1977 Effects of orally administered oestradiol decanoate on plasma oestradiol oestrone and gonadotrophin levels vaginal cytology cervical mucus and endometrium in ovariectomized women Clinical Endocrinology 7 1 73 77 doi 10 1111 j 1365 2265 1977 tb02941 x PMID 880735 S2CID 13639429 a b Luisi M Kicovic PM Alicicco E Franchi F April 1978 Effects of estradiol decanoate in ovariectomized women Journal of Endocrinological Investigation 1 2 101 106 doi 10 1007 BF03350355 PMID 755846 S2CID 38187367 a b Chaudhury RR 1 January 1981 Pharmacology of Estrogens Elsevier Science amp Technology Books p 36 ISBN 978 0 08 026869 9 Jameson JL De Groot LJ 25 February 2015 Endocrinology Adult and Pediatric E Book Elsevier Health Sciences pp 2387 ISBN 978 0 323 32195 2 Nieschlag E Behre HM 6 December 2012 Testosterone Action Deficiency Substitution Springer Science amp Business Media pp 300 ISBN 978 3 642 72185 4 a b c d e f Leyendecker G Geppert G Nocke W Ufer J May 1975 Estradiol 17beta estrone LH and FSH in serum after administration of estradiol 17beta estradiolbenzoate estradiol valeriate and estradiol undecylate in the female author s transl Estradiol 17b estrone LH and FSH in serum after administration of estradiol 17b estradiol benzoate estradiol valeriate and estradiol undecylate in the female Geburtshilfe und Frauenheilkunde in German 35 5 370 374 PMID 1150068 Burdock GA 1997 Encyclopedia of Food and Color Additives CRC Press pp 2870 ISBN 978 0 8493 9412 6 Junkmann K 1957 Long acting steroids in reproduction Recent Progress in Hormone Research 13 389 419 discussion 419 28 PMID 13477813 Junkmann K Witzel H 1957 Chemistry and pharmacology of steroid hormone esters Chemistry and pharmacology of steroid hormone esters Zeitschrift Fur Vitamin Hormon und Fermentforschung in German 9 1 2 97 143 contd PMID 13531579 Archived from the original on 2018 11 23 Retrieved 2018 11 23 Armstrong NA James KC 1980 Drug release from lipid based dosage forms I International Journal of Pharmaceutics 6 3 4 185 193 doi 10 1016 0378 5173 80 90103 9 Saygin D Tabib T Bittar HE Valenzi E Sembrat J Chan SY et al 1953 Transcriptional profiling of lung cell populations in idiopathic pulmonary arterial hypertension Over protracted effective estrogens Pulmonary Circulation in German 10 1 doi 10 1007 BF00246561 PMC 7052475 PMID 32166015 S2CID 20753905 17 undecenoate of estradiol Saygin D Tabib T Bittar HE Valenzi E Sembrat J Chan SY et al 1967 Transcriptional profiling of lung cell populations in idiopathic pulmonary arterial hypertension Pulmonary Circulation 10 1 107 127 doi 10 1080 00224496709550519 PMC 7052475 PMID 32166015 von Bruchhausen F Dannhardt G Ebel S Frahm AW Hackenthal E Holzgrabe U 2 July 2013 Hagers Handbuch der Pharmazeutischen Praxis Band 8 Stoffe E O Springer Verlag pp 84 ISBN 978 3 642 57994 3 Boschann HW July 1958 Observations of the role of progestational agents in human gynecologic disorders and pregnancy complications Annals of the New York Academy of Sciences 71 5 727 752 Bibcode 1958NYASA 71 727B doi 10 1111 j 1749 6632 1958 tb46803 x PMID 13583829 Bishop PM 1962 Chemistry of the Sex Hormones Thomas p 78 a b el Mahgoub S Karim M February 1972 Depot estrogen as a monthly contraceptive in nulliparous women with mild uterine hypoplasia American Journal of Obstetrics and Gynecology 112 4 575 576 doi 10 1016 0002 9378 72 90319 5 PMID 5008627 a b Toppozada MK 1983 Monthly Injectable Contraceptives In Goldsmith A Toppozada M eds Long Acting Contraception pp 93 103 OCLC 35018604 Toppozada MK April 1994 Existing once a month combined injectable contraceptives Contraception 49 4 293 301 doi 10 1016 0010 7824 94 90029 9 PMID 8013216 Kadam SS July 2007 Principles of Medicinal Chemistry Volume 2 Pragati Books Pvt Ltd pp 381 ISBN 978 81 85790 03 9 Beck LR Cowsar DR Pope VZ July 1980 Long acting steroidal contraceptive systems PDF Research Frontiers in Fertility Regulation 1 1 1 16 PMID 12179628 S2CID 13863575 Karim M el Mahgoub S July 1971 Conception control by cyclic injections of norethisterone enanthate and estradiol unducelate American Journal of Obstetrics and Gynecology 110 5 740 742 doi 10 1016 0002 9378 71 90268 7 PMID 5563241 Retrieved from https en wikipedia org w index php title Estradiol undecylate amp oldid 1171819912, wikipedia, wiki, book, books, library,

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