Diethylstilbestrol














































































































Diethylstilbestrol

Diethylstilbestrol.svg

Diethylstilbestrol molecule ball.png
Clinical data
Synonyms
DES; Stilboestrol; Stilbestrol; (E)-11,12-Diethyl-4,13-stilbenediol

AHFS/Drugs.com

Micromedex Detailed Consumer Information
Pregnancy
category


  • X


Routes of
administration

By mouth, vaginal, topical, intravenous, intramuscular injection (as an ester)
Drug class
Nonsteroidal estrogen
ATC code

  • G03CB02 (WHO) G03CC05 (WHO), L02AA01 (WHO)


Pharmacokinetic data
Bioavailability
Well-absorbed[1]
Metabolism
Glucuronidation, oxidation[1]
Metabolites
• (Z,Z)-Dienestrol[1]
• Paroxypropione[1]
Elimination half-life

24 hours[1]
Identifiers


CAS Number

  • 56-53-1 ☑Y


PubChem CID

  • 448537

IUPHAR/BPS
  • 2801

DrugBank

  • DB00255 ☑Y

ChemSpider

  • 395306 ☑Y

UNII
  • 731DCA35BT

KEGG

  • D00577 ☑Y

ChEBI

  • CHEBI:41922 ☑Y

ChEMBL

  • CHEMBL411 ☑Y

ECHA InfoCard
100.000.253 Edit this at Wikidata
Chemical and physical data
Formula
C18H20O2
Molar mass
268.356 g/mol
3D model (JSmol)
  • Interactive image






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Diethylstilbestrol (DES), also known as stilbestrol or stilboestrol, is an estrogen medication which is mostly no longer used.[2][3] In the past, it was widely used for a variety of indications including pregnancy support for women with a history of recurrent miscarriage, hormone therapy for menopausal symptoms and estrogen deficiency in women, treatment of prostate cancer in men and breast cancer in women, and other uses. While most commonly taken by mouth, DES was available for use by other routes as well, for instance vaginal, topical, and by injection.


DES is an estrogen, or an agonist of the estrogen receptors, the biological target of estrogens like estradiol.[3] It is a synthetic and nonsteroidal estrogen of the stilbestrol group, and differs from the natural estrogen estradiol in various ways.[3] Compared to estradiol, DES has greatly improved bioavailability when taken by mouth, is more resistant to metabolism, and shows relatively increased effects in certain parts of the body like the liver and uterus.[3] These differences result in DES having an increased risk of blood clots, cardiovascular issues, and certain other adverse effects.[3]


DES was discovered in 1938.[4] From about 1940 to 1971, the medication was given to pregnant women in the incorrect belief it would reduce the risk of pregnancy complications and losses.[4] In 1971, DES was shown to cause clear cell carcinoma, a rare vaginal tumor, in girls and women who had been exposed to this medication in utero.[4] The United States Food and Drug Administration subsequently withdrew approval of DES as a treatment for pregnant women.[4] Follow-up studies have indicated that DES also has the potential to cause a variety of significant adverse medical complications during the lifetimes of those exposed.[4][5]


The United States National Cancer Institute recommends[6] women born to mothers who took DES undergo special medical exams on a regular basis to screen for complications as a result of the medication. Individuals who were exposed to DES during their mothers' pregnancies are commonly referred to as "DES daughters" and "DES sons".[4][7] Since the discovery of the toxic effects of DES, it has largely been discontinued and is now mostly no longer marketed.[4][8]





Contents






  • 1 Medical uses


  • 2 Side effects


    • 2.1 Long-term effects




  • 3 Overdose


  • 4 Pharmacology


    • 4.1 Pharmacodynamics


      • 4.1.1 Estrogenic activity


      • 4.1.2 Antigonadotropic effects


      • 4.1.3 Other activities




    • 4.2 Pharmacokinetics




  • 5 Chemistry


  • 6 History


    • 6.1 Synthesis


    • 6.2 Clinical use


    • 6.3 Lawsuits




  • 7 Society and culture


  • 8 Veterinary use


    • 8.1 Canine incontinence


    • 8.2 Livestock growth promotion




  • 9 References


  • 10 Further reading


  • 11 External links





Medical uses


DES has been used in the past for the following indications:




  • Recurrent miscarriage in pregnancy


  • Menopausal hormone therapy for the treatment of menopausal symptoms such as hot flashes and vaginal atrophy


  • Hormone therapy for hypoestrogenism (e.g., gonadal dysgenesis, premature ovarian failure, and after oophorectomy)


  • Postpartum lactation suppression to prevent or reverse breast engorgement


  • Gonorrheal vaginitis (discontinued following the introduction of the antibiotic penicillin)


  • Prostate cancer and breast cancer

  • Prevention of tall stature in tall adolescent girls

  • As an emergency postcoital contraceptive

  • As a means of chemical castration for hypersexuality and paraphilias in men and sex offenders.


Interest in the use of DES to treat prostate cancer in men continues today.[9][10][11][12][13][14][15] However, some researchers have advocated for the use of bioidentical parenteral estrogens like polyestradiol phosphate in favor of oral synthetic estrogens like DES due to their much lower risk of cardiovascular toxicity.[16][13][15] In addition to prostate cancer, some interest in the use of DES to treat breast cancer in women continues today as well.[17][18] However, similarly to the case of prostate cancer, some researchers have argued for the use bioidentical estrogens like estradiol instead of DES for breast cancer.[17][19]



Side effects


At doses above 1 mg/day by mouth, DES is associated with high rates of side effects including nausea, vomiting, abdominal discomfort, headache, and bloating, with an incidence of 15 to 50%.[20]


In studies of DES as a form of high-dose estrogen therapy for men with prostate cancer, it has been associated with considerable cardiovascular morbidity and mortality.[10] The risk is dose-dependent.[10] A dosage of 5 mg/day DES has been associated with a 36% increase in non-cancer-related (mostly cardiovascular) deaths.[10] In addition, there is an up to 15% incidence of venous thromboembolism.[21] A 3 mg/day dosage of DES has been associated with an incidence of thromboembolism of 9.6 to 17%, with an incidence of cardiovascular complications of 33.3%.[10] A lower dosage of 1 mg/day DES has been associated with a rate of death due to cardiovascular events of 14.8% (relative to 8.3% for orchiectomy alone).[10]


In men treated with it for prostate cancer, DES has been found to produce high rates of gynecomastia (breast development) of 41 to 77%.[22]



Long-term effects



DES has been linked to a variety of long-term adverse effects, such as increased risk of vaginal clear-cell adenocarcinoma, vaginal adenosis, T-shaped uterus, uterine fibroids, incompetent cervix, breast cancer, infertility, hypogonadism, intersex defects, depression, and others, in women who were treated with it during pregnancy and/or in their offspring.[23]



Overdose


DES has been assessed in the past in clinical studies at extremely high dosages of as much as 1,500 mg/day.[17][24]



Pharmacology



Pharmacodynamics



Estrogenic activity


DES is an estrogen; specifically, it is a highly potent full agonist of both of the estrogen receptors (ERs).[25][26] It has approximately 468% and 295% of the affinity of estradiol at the ERα and ERβ, respectively.[27] However, EC50 values of 0.18 nM and 0.06 nM of DES for the ERα and ERβ, respectively, have been reported, suggesting, in spite of its binding affinity for the two receptors, several-fold preference for activation of the ERβ over the ERα.[28]


A dosage of 1 mg/day DES is approximately equivalent to a dosage of 50 µg/day ethinylestradiol in terms of systemic estrogenic potency.[1] Similarly to ethinylestradiol, DES shows a marked and disproportionately strong effect on liver protein synthesis.[3] Whereas its systemic estrogenic potency was about 3.8-fold of that of estropipate (piperazine estrone sulfate), which has similar potency to micronized estradiol, the hepatic estrogenic potency of DES was 28.4-fold that of estropipate (or about 7.5-fold stronger potency for a dosage with equivalent systemic estrogenic effect).[1]


DES has at least three mechanisms of action in the treatment of prostate cancer in men.[29] It suppresses gonadal androgen production and hence circulating androgen levels due to its antigonadotropic effects; it stimulates hepatic sex hormone-binding globulin (SHBG) production, thereby increasing circulating levels of SHBG and decreasing the free fraction of testosterone and dihydrotestosterone (DHT) in the circulation; and it may have direct cytotoxic effects in the testes and prostate gland.[29] DES has also been found to decrease DNA synthesis at high doses.[29]






































































































































Relative oral potencies of estrogens
Estrogen Type HF VE UCa FSH LH
HDL-C
SHBG CBG AGT
Ratio
Estradiol Bioidentical 1.0 1.0 1.0 1.0 1.0 1.0 1.0 1.0 1.0 1.0
Estrone Bioidentical ND ND ND 0.3 0.3 ND ND ND ND
ND
Estriol Bioidentical 0.3 0.3 0.1 0.3 ND 0.2 ND ND ND 0.67
Estrone sulfate Bioidentical ND 0.9 0.9 0.9 0.9 0.5 0.9 0.7 1.5 0.56–1.7
Conjugated estrogens Natural 1.2 1.5 2.0 1.1 1.0 1.5 3.0 1.5 5.0 1.3–4.5
Equilin sulfate Natural ND ND ND ND ND 6.0 7.5 6.0 7.5
ND
Ethinylestradiol Synthetic 120 150 40 120 100 400 500 600 350 2.9–5.0
Diethylstilbestrol Synthetic ND ND ND 3.4 ND ND 25.6 24.5 19.5 5.7–7.5

Notes: Values are ratios, with estradiol as standard (i.e., 1.0). Abbreviations: HF = Clinical relief of hot flashes. VE = Increased proliferation of vaginal epithelium. UCa = Decrease in UCa. FSH = Suppression of FSH levels. LH = Suppression of LH levels. HDL-C, SHBG, CBG, and AGT = Increase in the serum levels of these hepatic proteins. Ratio = Ratio of liver protein effects to hot flashes relief and gonadotropin suppression. ND = No data. Type: Bioidentical = Identical to those found in humans. Natural = Naturally occurring but not identical to those found in humans (e.g., estrogens of other species). Synthetic = Man-made, does not naturally occur in animals or in the environment. Miscellaneous: Direct link to table. Sources: [30][31][32][33][34][35]






































































































Oral potencies of estrogens
Estrogen Type
EPD
(mg/14 days)

EPD
(mg/day)

MSD
(mg/14 days)

MSD
(mg/day)

Estradiol (micronized)
Bioidentical 60 4.3 14–28 1.0–2.0
Estradiol valerate Bioidentical 60 4.3 14–28 1.0–2.0
Estriol Bioidentical 140–150a
10.0–10.7a
28–84 2.0–6.0
Estriol succinate Bioidentical 140–150a
10.0–10.7a
28–84 2.0–6.0
Conjugated estrogens Natural 60 4.3 8.4–17.5 0.6–1.25
Ethinylestradiol Synthetic 1.0–1.5 0.071–0.11 0.28 0.02
Mestranol Synthetic 1.5–1.8 0.11–0.13 0.35 0.025
Quinestrol Synthetic 2.0–4.0 0.14–0.29 ND
ND
Diethylstilbestrol Synthetic 20–30 1.4–2.1 ND
ND
Diethylstilbestrol dipropionate Synthetic 15–20 1.1–1.4 ND
ND
Dienestrol diacetate Synthetic 40–60 2.9–4.3 ND
ND

Addendum: The ovulation-inhibiting dose (OID) of ethinylestradiol is 0.1 mg/day.[36]Footnotes: a = Taken in divided doses three times per day. Abbreviations: EPD = Endometrial proliferation dose. MSD = Menopausal substitution dose. Miscellaneous: Direct link to table. Sources: [37][31][38][39]






















































Parenteral potencies of estrogens
Estrogen Type
EPD (14 days)
Duration
Estradiol benzoate Bioidentical 25–30 mg 5 mg ≈ 5 days
Estradiol dipropionate Bioidentical 25–30 mg 5 mg ≈ 5–8 days
Estradiol valerate Bioidentical 20 mg 10 mg ≈ 14 days
Estradiol cypionate Bioidentical 25–30 mg 5 mg ≈ 14 days
Polyestradiol phosphate Bioidentical 40–60 mg 40 mg ≈ 28 days
Diethylstilbestrol Synthetic 20 mg 3 mg ≈ 3 days
Diethylstilbestrol dipropionate Synthetic 15 mg 2.5 mg ≈ 5 days

Addendum: An effective ovulation-inhibiting dose of estradiol undecylate is 20–30 mg/month.[40]Notes: All of the estrogens are by intramuscular injection. Abbreviations: EPD = Endometrial proliferation dose. Miscellaneous: Direct link to table. Sources: [41][42]


Antigonadotropic effects


Due to its estrogenic activity, DES has antigonadotropic effects.[29][43][44] That is, it exerts negative feedback on the hypothalamic–pituitary–gonadal axis (HPG axis), suppresses the secretion of the gonadotropins, luteinizing hormone (LH) and follicle-stimulating hormone (FSH), and suppresses sex hormone production as well as gamete production or maturation in the gonads.[29][43][44] DES suppresses testosterone levels in men into the castrate range (<50 ng/dL) within 1 to 2 weeks at doses of 3 mg/day and above.[44] Conversely, a dosage of 1 mg/day DES is unable to fully suppress testosterone levels into the castrate range in men, which instead often stabilize at just above castrate levels (>50 ng/dL).[10][29][43]



Other activities


In addition to the ERs, an in vitro study found that DES also possesses activity, albeit relatively weak, at a variety of other steroid hormone receptors.[28] Whereas the study found EC50 values of 0.18 nM and 0.06 nM of DES for the ERα and ERβ, respectively, the drug showed significant glucocorticoid activity at a concentration of 1 μM that surpassed that of 0.1 nM dexamethasone as well as significant antagonism of the androgen, progesterone, and mineralocorticoid receptors (75%, 85%, and 50% inhibition of positive control stimulation, respectively, at a concentration of 1 μM).[28] It also showed approximately 25% inhibition of the activation of PPARγ and LXRα at a concentration of 10 μM.[28] The researchers stated that, to the best of their knowledge, they were the first to report such actions of DES, and hypothesized that these actions could be involved in the clinical effects of DES, for instance, in prostate cancer (notably in which particularly high dosages of DES are employed).[28] However, they also noted that the importance of the activities requires further study in animal models at pharmacologically relevant doses.[28]


DES has been identified as an antagonist of all three isotypes of the estrogen-related receptors (ERRs), the ERRα, ERRβ, and ERRγ.[45]



Pharmacokinetics


DES is well-absorbed with oral administration.[1] With an oral dosage of 1 mg/day DES, plasma levels of DES at 20 hours following the last dose ranged between 0.9 to 1.9 ng/mL (3.4 to 7.1 nmol/L).[1] The distribution half-life of DES is 80 minutes.[1] It has no affinity for SHBG or corticosteroid-binding globulin, and hence is not bound to these proteins in the circulation.[46] DES is metabolized mainly by glucuronidation and oxidation, with the latter including aromatic hydroxylation of the ethyl side chains and dehydrogenation into (Z,Z)-dienestrol.[1] It is also known to produce paroxypropione as a metabolite.[47] DES produces transient quinone-like reactive intermediates that cause cellular and genetic damage, which may explain the known carcinogenic effects of DES in humans.[1] However, other research suggests that the toxic effects of DES may simply be due to overactivation of the ERs.[48] The elimination half-life of DES is 24 hours.[1]



Chemistry




Chemical structures of estradiol and DES.[49] Note the preservation of the two hydroxyl groups in DES and the similar distance between them relative to estradiol, which is notable when it is considered that DES was discovered serendipitously.[49][50][51]


DES belongs to the stilbestrol (4,4'-dihydroxystilbene) group of compounds.[52] It is a nonsteroidal open-ring analogue of the steroidal estrogen estradiol.[49] DES was derived from the naturally occurring compound anethole, a weakly estrogenic constituent of anise and fennel.[52][53][51][50] Anethole was demethylated to form anol and anol then spontaneously dimerized into dianol and hexestrol, with DES subsequently being synthesized via structural modification of hexestrol.[52][53][51][50] It has been determined via X-ray crystallography that the molecular dimensions of DES are almost identical to those of estradiol, particularly in regards to the distance between the hydroxyl groups at either end of the molecules.[50]



History



Synthesis


DES was first synthesized in early 1938 by Leon Golberg, then a graduate student of Sir Robert Robinson at the Dyson Perrins Laboratory at the University of Oxford. Golberg's research was based on work by Wilfrid Lawson at the Courtauld Institute of Biochemistry, (led by Sir Edward Charles Dodds at Middlesex Hospital Medical School now part of University College London). A report of its synthesis was published in Nature on 5 February 1938.[54][55][56]


DES research was funded by the UK Medical Research Council (MRC), which had a policy against patenting drugs discovered using public funds. Because it was not patented, DES was produced by more than 200 pharmaceutical and chemical companies worldwide.



Clinical use


DES (in tablets up to 5 mg) was approved by the United States Food and Drug Administration (FDA) on September 19, 1941 for four indications: gonorrheal vaginitis, atrophic vaginitis, menopausal symptoms, and postpartum lactation suppression to prevent breast engorgement.[56] The gonorrheal vaginitis indication was dropped when the antibiotic penicillin became available. From its very inception, the drug was highly controversial.[57][58]


In 1941, Charles Huggins and Clarence Hodges at the University of Chicago found DES to be the first effective drug for the treatment of metastatic prostate cancer.[59][60]


Orchiectomy or DES or both were the standard initial treatment for symptomatic advanced prostate cancer for over 40 years, until the GnRH agonist leuprorelin was found to have efficacy similar to DES without estrogenic effects and was approved in 1985.[61]


From the 1940s until the late 1980s, DES was FDA-approved as estrogen-replacement therapy for estrogen deficiency states such as ovarian dysgenesis, premature ovarian failure, and after oophorectomy.


In the 1940s, DES was used off-label to prevent adverse pregnancy outcomes in women with a history of miscarriage. On July 1, 1947, the FDA approved the use of DES for this indication. The first such approval was granted to Bristol-Myers Squibb, allowing use of 25 mg (and later 100 mg) tablets of DES during pregnancy. Approvals were granted to other pharmaceutical companies later in the same year.[62] The recommended regimen started at 5 mg per day in the seventh and eighth weeks of pregnancy (from first day of last menstrual period), increased every other week by 5 mg per day through the 14th week, and then increased every week by 5 mg per day from 25 mg per day in the 15th week to 125 mg per day in the 35th week of pregnancy.[63]
DES was originally considered effective and safe for both the pregnant woman and the developing baby. It was aggressively marketed and routinely prescribed. Sales peaked in 1953.


In the early 1950s, a double-blind clinical trial at the University of Chicago assessed pregnancy outcomes in women who were assigned to either receive or not receive DES.[64]
The study showed no benefit of taking DES during pregnancy; adverse pregnancy outcomes were not reduced in the women who were given DES. By the late 1960s, six of seven leading textbooks of obstetrics said DES was ineffective at preventing miscarriage.[62][65]


Despite an absence of evidence supporting the use of DES to prevent adverse pregnancy outcomes, DES continued to be given to pregnant women through the 1960s. In 1971, a report published in the New England Journal of Medicine showed a probable link between DES and vaginal clear cell adenocarcinoma in girls and young women who had been exposed to this drug in utero. Later in the same year, the FDA sent an FDA Drug Bulletin to all U.S. physicians advising against the use of DES in pregnant women. The FDA also removed prevention of miscarriage as an indication for DES use and added pregnancy as a contraindication for DES use.[66] On February 5, 1975, the FDA ordered 25 mg and 100 mg tablets of DES withdrawn, effective February 18, 1975.[67] The number of persons exposed to DES during pregnancy or in utero during 1940–1971 is unknown, but may be as high as 2 million in the United States. DES was also used in other countries, most notably France, the Netherlands, and Great Britain.


From the 1950s through the beginning of the 1970s, DES was prescribed to prepubescent girls to begin puberty and thus stop growth by closing growth plates in the bones. Despite its clear link to cancer, doctors continued to recommend the hormone for "excess height".[68]


In 1960, DES was found to be more effective than androgens in the treatment of advanced breast cancer in postmenopausal women.[69] DES was the hormonal treatment of choice for advanced breast cancer in postmenopausal women until 1977, when the FDA approved tamoxifen, a selective estrogen receptor modulator with efficacy similar to DES but fewer side effects.[70]


Several sources from medical literature in the 1970s and 1980s indicate that DES was used for treatment of transgender individuals.[71][72][73]


In 1973, in an attempt to restrict off-label use of DES as a postcoital contraceptive (which had become prevalent at many university health services following publication of an influential study in 1971 in JAMA) to emergency situations such as rape, an FDA Drug Bulletin was sent to all U.S. physicians and pharmacists that said the FDA had approved, under restricted conditions, postcoital contraceptive use of DES.[74]


In 1975, the FDA said it had not actually given (and never did give) approval to any manufacturer to market DES as a postcoital contraceptive, but would approve that indication for emergency situations such as rape or incest if a manufacturer provided patient labeling and special packaging as set out in a FDA final rule published in 1975.[75] To discourage off-label use of DES as a postcoital contraceptive, the FDA in 1975 removed DES 25 mg tablets from the market and ordered the labeling of lower doses (5 mg and lower) of DES still approved for other indications changed to state: "This drug product should not be used as a postcoital contraceptive" in block capital letters on the first line of the physician prescribing information package insert and in a prominent and conspicuous location of the container and carton label.[67][76] In the 1980s, off-label use of the Yuzpe regimen of certain regular combined oral contraceptive pills superseded off-label use of DES as a postcoital contraceptive.[77]


In 1978, the FDA removed postpartum lactation suppression to prevent breast engorgement from their approved indications for DES and other estrogens.[78] In the 1990s, the only approved indications for DES were treatment of advanced prostate cancer and treatment of advanced breast cancer in postmenopausal women. The last remaining U.S. manufacturer of DES, Eli Lilly, stopped making and marketing it in 1997.



Lawsuits


In the 1970s, the negative publicity surrounding the discovery of DES's long-term effects resulted in a huge wave of lawsuits in the United States against its manufacturers. These culminated in a landmark 1980 decision of the Supreme Court of California, Sindell v. Abbott Laboratories, in which the court imposed a rebuttable presumption of market share liability upon all DES manufacturers, proportional to their share of the market at the time the drug was consumed by the mother of a particular plaintiff.


A lawsuit was filed in Boston Federal Court by 53 DES daughters who say their breast cancers were the result of DES being prescribed to their mothers while pregnant with them. Their cases survived a Daubert hearing. In 2013, the Fecho sisters who initiated the breast cancer/DES link litigation agreed to an undisclosed settlement amount on the second day of trial. The remaining litigants have received various settlements.[79]



Society and culture


Alan Turing, the ground breaking cryptographer, founder of computing science and programmable computers, who also proposed the actual theoretical model of biological morphogenesis, was forced onto the medication to induce chemical castration as a punitive "treatment" for homosexual behaviour, shortly before he died in ambiguous circumstances.[80]



Veterinary use



Canine incontinence


DES has been very successful in treating female canine incontinence stemming from poor sphincter control. It is still available from compounding pharmacies, and at the low (1 mg) dose, does not have the carcinogenic properties that were so problematic in humans.[81] It is generally administered once a day for seven to ten days and then once every week as needed.



Livestock growth promotion


The greatest usage of DES was in the livestock industry, used to improve feed conversion in beef and poultry. During the 1960s, DES was used as a growth hormone in the beef and poultry industries. It was later found to cause cancer by 1971, but was not phased out until 1979.[82][83] When DES was discovered to be harmful to humans, it was moved to veterinary use.



References





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Further reading



  • Johnston, Emily (2017). "Poisoned subjects: life writing of DES daughters". Frontiers: A Journal of Women Studies. University of Nebraska Press. 38 (1): 31&ndash, 63. JSTOR 10.5250/fronjwomestud.38.1.0031.


External links



  • National Cancer Institute DES information


  • DES Update from the U.S. Centers for Disease Control and Prevention


  • DES Action USA national consumer organization providing comprehensive information for DES-exposed individuals


  • DES Booklets from the U.S. National Institutes of Health (circa 1980)


  • DES Follow-up Study National Cancer Institute's longterm study of DES-exposed persons (including the DES-AD Project)


  • University of Chicago DES Registry of patients with CCA (clear cell adenocarcinoma) of the vagina and/or cervix.


  • DES Diethylstilbestrol Provides resources and social media links for general DES awareness













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