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Wikipedia

Norethisterone

January 01, 1970

Norethisterone, also known as norethindrone and sold under many brand names, is a progestin medication used in birth control pills, menopausal hormone therapy, and for the treatment of gynecological disorders.[3][5] The medication is available in both low-dose and high-dose formulations and both alone and in combination with an estrogen.[5][6] It is used by mouth or, as norethisterone enanthate, by injection into muscle.[3][5][7]

Norethisterone
Clinical data
Trade namesMany
Other namesNET; Norethindrone; NSC-9564; LG-202; Ethinylnortestosterone; Norpregneninolone; Anhydrohydroxy-norprogesterone; Ethinylestrenolone; 17α-Ethynyl-19-nortestosterone; 17α-Ethynylestra-4-en-17β-ol-3-one; 17α-Hydroxy-19-norpregn-4-en-20-yn-3-one
AHFS/Drugs.comMonograph
MedlinePlusa604034
License data
Routes of
administration		By mouth, intramuscular injection (as NETETooltip norethisterone enanthate)
Drug classProgestogen (medication); Progestin
ATC code
Legal status
Legal status
Pharmacokinetic data
Bioavailability47–73% (mean 64%)[1][2]
Protein binding97%:[3]
Albumin: 61%;[3]
SHBGTooltip Sex hormone-binding globulin: 36%[3]
MetabolismMainly CYP3A4 (liver);[4] also 5α-/5β-reductase, 3α-Tooltip 3α-hydroxysteroid dehydrogenase/3β-HSDTooltip 3β-hydroxysteroid dehydrogenase, and aromatase
Elimination half-life5.2–12.8 hours (mean 8.0 hours)[1]
Identifiers
  • (8R,9S,10R,13S,14S,17R)-17-ethynyl-17-hydroxy-13-methyl-1,2,6,7,8,9,10,11,12,14,15,16-dodecahydrocyclopenta[a]phenanthren-3-one
CAS Number
  • 68-22-4 Y
PubChem CID
  • 6230
IUPHAR/BPS
  • 2880
DrugBank
  • DB00717 Y
ChemSpider
  • 5994 Y
UNII
  • T18F433X4S
KEGG
  • D00182 Y
ChEBI
  • CHEBI:7627 Y
ChEMBL
  • ChEMBL1162 Y
CompTox Dashboard (EPA)
  • DTXSID9023380
ECHA InfoCard100.000.619
Chemical and physical data
FormulaC20H26O2
Molar mass298.426 g·mol−1
3D model (JSmol)
  • Interactive image
Melting point203 to 204 °C (397 to 399 °F)
  • C[C@]12CC[C@H]3[C@H]([C@@H]1CC[C@]2(C#C)O)CCC4=CC(=O)CC[C@H]34
  • InChI=1S/C20H26O2/c1-3-20(22)11-9-18-17-6-4-13-12-14(21)5-7-15(13)16(17)8-10-19(18,20)2/h1,12,15-18,22H,4-11H2,2H3/t15-,16+,17+,18-,19-,20-/m0/s1 Y
  • Key:VIKNJXKGJWUCNN-XGXHKTLJSA-N Y
  (verify)

Side effects of norethisterone include menstrual irregularities, headaches, nausea, breast tenderness, mood changes, acne, increased hair growth.[8][9] Norethisterone is a progestin, or a synthetic progestogen, and hence is an agonist of the progesterone receptor, the biological target of progestogens like progesterone.[3][5] It has weak androgenic and estrogenic activity, mostly at high dosages, and no other important hormonal activity.[3][10]

Norethisterone was discovered in 1951 and was one of the first progestins to be developed.[11][12][13] It was first introduced for medical use on its own in 1957 and was introduced in combination with an estrogen for use as a birth control pill in 1963.[13][14] It is sometimes referred to as a "first-generation" progestin.[15][16] Along with desogestrel, it is one of the only progestins that is widely available as a progestogen-only "mini pill" for birth control.[17][18] Norethisterone is marketed widely throughout the world.[19] It is available as a generic medication.[20] In 2021, it was the 140th most commonly prescribed medication in the United States, with more than 4 million prescriptions.[21][22] It is on the World Health Organization's List of Essential Medicines.[23]

Medical uses edit

Norethisterone is used as a hormonal contraceptive in combination with an estrogen – usually ethinylestradiol (EE) – in combined oral contraceptive pills and alone in progestogen-only pills.

Another medical use of norethisterone is to alleviate endometriosis related pain. In fact, 50% of patients who received medical or surgical treatment for endometriosis-related pelvic pain have benefited from progestin therapy. This could be due to the fact that norethisterone induces endometrial proliferation during secretory phase, which has been shown to alleviate endometrial pain complaints. Another way in which norethisterone may be acting to reduce endometrial pain is via inhibition of ovulation. Endometriosis pain and discomfort is worse during ovulation.[24]

Formulations and brand names of norethisterone and esters
Composition Dose Brand names Use
NET only Low (e.g., 0.35 mg) Multiple[a] Progestogen-only oral contraceptive
NET or NETA only High (e.g., 5 mg, 10 mg) Multiple[b] Gynecological disorders and other uses
NETE only Injection (e.g., 200 mg) Multiple[c] Progestogen-only injectable contraceptive
NET or NETA with ethinylestradiol Low (e.g., 0.4 mg, 0.5 mg, 0.75 mg, 1 mg, 1.5 mg) Multiple[d] Combined oral contraceptive
NET with mestranol Low (e.g., 1 mg, 2 mg) Multiple[e] Combined oral contraceptive
NETA with estradiol Low (e.g., 0.1 mg, 0.5 mg) Multiple[f] Combined menopausal hormone therapy
NETE with estradiol valerate Injection (e.g., 50 mg) Multiple[g] Combined injectable contraceptive
Abbreviations: NET = Norethisterone. NETA = Norethisterone acetate. NETE = Norethisterone enanthate.
Sources: [25][26] [27][28]
Notes:
  1. ^ Camila, Errin, Heather, Jencycla, Jolivette, Locilan, Micro-Novum, Micronovum, Micronor, Nor-QD, Nora, Noriday, Ortho Micronor
  2. ^ Aygestin, Lupaneta Pack (combination pack with leuprorelin), Norcolut, Norlutate, Primolut N, Primolut Nor, SH-420, Utovlan
  3. ^ Depocon, Doryxas, NET-EN, Noristerat, Norigest, Nur-Isterate
  4. ^ Aranelle, Balziva, Binovum, Brevicon, Brevinor, Briellyn, Cyclafem, Dasetta, Estrostep, Femcon, Generess, Gildagia, Gildess, Jinteli, Junel, Larin, Leena, Lo Loestrin, Lo Minastrin, Loestrin, Lolo, Lomedia, Microgestin, Minastrin, Modicon, Nelova, Norimin, Norinyl, Nortrel, Ortho, Ortho-Novum, Ovcon, Ovysmen, Philith, Primella, Select, Synphase, Synphasic, Tilia, Tri-Legest, Tri-Norinyl, Trinovum, Vyfemla, Wera, Wymzya, Zenchent, Zeosa
  5. ^ Norethin, Noriday, Norinyl, Norquen, Ortho-Novum, Sophia
  6. ^ Activella, Activelle, Alyacen, Cliane, Climagest, Climesse, Cliovelle, CombiPatch, Elleste Duet, Estalis, Estropause, Eviana, Evorel, Kliane, Kliofem, Kliogest, Kliovance, Mesigyna, Mesygest, Mimvey, Necon, Novofem, Nuvelle, Sequidot, Systen, Trisequens
  7. ^ Chinese Injectable No. 3, Efectimes, Ginediol, Mesigyna, Mesilar, Meslart, Mesocept, Mesygest, Nofertyl, Nofertyl Lafrancol, Noregyna, Norestrin, Norifam, Norigynon, Nostidyn, Sexseg, Solouna

Contraindications edit

High-dose (10 mg/day) norethisterone has been associated with hepatic veno-occlusive disease, and because of this adverse effect, norethisterone should not be given to patients undergoing allogeneic bone marrow transplantation, as it has been associated with substantially lower one-year survival post-transplantation.[29]: 217 [30]

Side effects edit

At contraceptive and hormone replacement dosages (0.35 to 1 mg/day), norethisterone has essentially progestogenic side effects only. In most clinical studies of norethisterone for contraception or menopausal hormone therapy, the drug has been combined with an estrogen, and for this reason, it is difficult to determine which of the side effects were caused by norethisterone and which of them were caused by estrogen in such research. However, NETE, an intramuscularly administered prodrug of norethisterone which is used as a long-acting contraceptive, is used without an estrogen, and hence can be employed as a surrogate for norethisterone in terms of understanding its effects and tolerability. In clinical studies, the most common side effect with NETE has been menstrual disturbances, including prolonged bleeding or spotting and amenorrhea.[29]: 253  Other side effects have included periodic abdominal bloating and breast tenderness, both of which are thought to be due to water retention and can be relieved with diuretics.[29]: 253  There has been no association with weight gain, and blood pressure, blood clotting, and glucose tolerance have all remained normal.[29]: 253  However, a decrease in HDL cholesterol has been observed.[29]: 253 

At high doses (5 to 60 mg/day), for instance those used in the treatment of gynecological disorders, norethisterone can cause hypogonadism due to its antigonadotropic effects and can have estrogenic and weak androgenic side effects.

High doses of NETA (10 mg/day) have been associated with abnormal liver function tests, including significant elevations in liver enzymes.[31][32][33] These liver enzymes included lactate dehydrogenase and glutamate pyruvate transaminase.[33] Although they were described as having no clinical relevance,[33] the elevated liver enzymes associated with NETA may have precluded its further development for male hormonal contraception.[31][32]

Androgenic edit

Due to its weak androgenic activity, norethisterone can produce androgenic side effects such as acne, hirsutism, and voice changes of slight severity in some women at high dosages (e.g., 10 to 40 mg/day).[9] This is notably not the case with combined oral contraceptives that contain norethisterone and EE, however.[10] Such formulations contain low dosages of norethisterone (0.35 to 1 mg/day)[10] in combination with estrogen and are actually associated with improvement in acne symptoms.[34][35] In accordance, they are in fact approved by the FDATooltip Food and Drug Administration for the treatment of acne in women in the United States.[34][35] The improvement in acne symptoms is believed to be due to a 2- to 3-fold increase in sex hormone-binding globulin (SHBG) levels and a consequent decrease in free testosterone levels caused by EE, which results in an overall decrease in androgenic signaling in the body.[36]

The sebaceous glands are highly androgen-sensitive and their size and activity are potential markers of androgenic effect.[37] A high dosage of 20 mg/day norethisterone or NETA has been found to significantly stimulate the sebaceous glands, whereas lower dosages of 5 mg/day and 2.5 mg/day norethisterone and NETA, respectively, did not significantly stimulate sebum production and were consequently regarded as devoid of significant androgenicity.[37] Conversely, dosages of norethisterone of 0.5 to 3 mg/day have been found to dose-dependently decrease SHBG levels (and hence to suppress hepatic SHBG production), which is another highly sensitive marker of androgenicity.[38]

A large clinical study of high to very high oral dosages of norethisterone (10 to 40 mg/day) administered for prolonged periods of time (4 to 35 weeks) to prevent miscarriage in pregnant women found that 5.5% of the women experienced mild androgenic side effects such as mild voice changes (hoarseness), acne, and hirsutism and that 18.3% of female infants born to the mothers showed, in most cases only slight, virilization of the genitals.[9] Maternal androgenic symptoms occurred most often in women who received a dosage of norethisterone of 30 mg/day or more for a period of 15 weeks or longer.[9] In the female infants who experienced virilization of the genitals, the sole manifestation in 86.7% of the cases was varied but almost always slight enlargement of the clitoris.[9] In the remaining 13.3% of the affected cases, marked clitoral enlargement and partial fusion of the labioscrotal folds occurred.[9] The dosages used in these cases were 20 to 40 mg/day.[9]

In a letter to the editor on the topic of virilization caused by high dosages of NETA in women, a physician expressed that they had not observed the "slightest evidence of virilization" and that there had "certainly been no hirsutism nor any voice changes" in 55 women with advanced breast cancer that they had treated with 30 to 60 mg/day norethisterone for up to six months.[39]

High-dosage norethisterone has been used to suppress menstruation in women with severe intellectual disability who were incapable of handling their own menses.[40][41] A study of 118 nulliparous women treated with 5 mg/day norethisterone for a period of 2 to 30 months found that the drug was effective in producing amenorrhea in 86% of the women, with breakthrough bleeding occurring in the remaining 14%.[40] Side effects including weight gain, hirsutism, acne, headache, nausea, and vomiting all did not appear to increase in incidence and no "disturbing side effects" were noted in any of the women.[40][41] Another study of 5 mg/day norethisterone in 132 women also made no mention of androgenic side effects.[42] These findings suggest little to no risk of androgenic side effects with norethisterone at a dosage of 5 mg/day.[40][41] A study of 194 women treated with 5 to 15 mg/day NETA for a median duration of 13 months of therapy to suppress symptoms of endometriosis observed no side effects in 55.2% of patients, weight gain in 16.1%, acne in 9.9%, mood lability in 8.9%, hot flashes in 8.3%, and voice deepening in two women (1.0%).[43]

Estrogenic edit

Norethisterone is weakly estrogenic (via conversion into its metabolite EE), and for this reason, it has been found at high dosages to be associated with high rates of estrogenic side effects such as breast enlargement in women and gynecomastia in men, but also with improvement of menopausal symptoms in postmenopausal women.[44] It has been suggested that very high dosages (e.g., 40 mg/day, which are sometimes used in clinical practice for various indications) of NETA (and by extension norethisterone) may result in an increased risk of venous thromboembolism (VTE) analogously to high dosages (above 50 μg/day) of EE, and that even doses of NETA of 10 to 20 mg, which correspond to EE doses of approximately 20 to 30 μg/day, may in certain women be associated with increased risk.[45][46] A study also found that ethinylestradiol and norethisterone had a greater influence on coagulation factors when the dose of norethisterone was 3 or 4 mg than when it was 1 mg.[47] This might have been due to additional ethinylestradiol generated by higher doses of norethisterone.[47]

Overdose edit

There have been no reports of serious side effects with overdose of norethisterone, even in small children.[48] As such, overdose usually does not require treatment.[48] High dosages of as much as 60 mg/day norethisterone have been studied for extended treatment durations without serious adverse effects described.[39]

Interactions edit

5α-Reductase plays an important role in the metabolism of norethisterone, and 5α-reductase inhibitors such as finasteride and dutasteride can inhibit its metabolism.[citation needed] Norethisterone is partially metabolized via hydroxylation by CYP3A4, and inhibitors and inducers of CYP3A4 can significantly alter circulating levels of norethisterone.[4] For instance, the CYP3A4 inducers rifampicin and bosentan have been found to decrease norethisterone exposure by 42% and 23%, respectively, and the CYP3A4 inducers carbamazepine and St. John's wort have also been found to accelerate norethisterone clearance.[4]

Pharmacology edit

Pharmacodynamics edit

Norethisterone is a potent progestogen and a weak androgen and estrogen.[3] That is, it is a potent agonist of the progesterone receptor (PR) and a weak agonist of the androgen receptor (AR) and the estrogen receptor (ER).[3] Norethisterone itself has insignificant affinity for the ER; its estrogenic activity is from an active metabolite that is formed in very small amounts, ethinylestradiol (EE), which is a very potent estrogen.[3] Norethisterone and its metabolites have negligible affinity for the glucocorticoid receptor (GR) and mineralocorticoid receptor (MR) and hence have no glucocorticoid, antiglucocorticoid, mineralocorticoid, or antimineralocorticoid activity.[3]

Relative affinities (%) of norethisterone, metabolites, and prodrugs
Compound Typea PRTooltip Progesterone receptor ARTooltip Androgen receptor ERTooltip Estrogen receptor GRTooltip Glucocorticoid receptor MRTooltip Mineralocorticoid receptor SHBGTooltip Sex hormone-binding globulin CBGTooltip Corticosteroid binding globulin
Norethisterone 67–75 15 0 0–1 0–3 16 0
5α-Dihydronorethisterone Metabolite 25 27 0 0 ? ? ?
3α,5α-Tetrahydronorethisterone Metabolite 1 0 0–1 0 ? ? ?
3α,5β-Tetrahydronorethisterone Metabolite ? 0 0 ? ? ? ?
3β,5α-Tetrahydronorethisterone Metabolite 1 0 0–8 0 ? ? ?
Ethinylestradiol Metabolite 15–25 1–3 112 1–3 0 0.18 0
Norethisterone acetate Prodrug 20 5 1 0 0 ? ?
Norethisterone enanthate Prodrug ? ? ? ? ? ? ?
Noretynodrel Prodrug 6 0 2 0 0 0 0
Etynodiol Prodrug 1 0 11–18 0 ? ? ?
Etynodiol diacetate Prodrug 1 0 0 0 0 ? ?
Lynestrenol Prodrug 1 1 3 0 0 ? ?
Notes: Values are percentages (%). Reference ligands (100%) were promegestone for the PRTooltip progesterone receptor, metribolone for the ARTooltip androgen receptor, estradiol for the ERTooltip estrogen receptor, dexamethasone for the GRTooltip glucocorticoid receptor, aldosterone for the MRTooltip mineralocorticoid receptor, dihydrotestosterone for SHBGTooltip sex hormone-binding globulin, and cortisol for CBGTooltip Corticosteroid-binding globulin. Footnotes: a = Active or inactive metabolite, prodrug, or neither of norethisterone. Sources: See template.

Progestogenic activity edit

Norethisterone is a potent progestogen and binds to the PR with approximately 150% of the affinity of progesterone.[3] In contrast, its parent compounds, testosterone, nandrolone (19-nortestosterone), and ethisterone (17α-ethynyltestosterone), have 2%, 22%, and 44% of the relative binding affinity of progesterone for the PR.[49] Unlike norethisterone, its major active metabolite 5α-dihydronorethisterone (5α-DHNET), which is formed by transformation via 5α-reductase, has been found to possess both progestogenic and marked antiprogestogenic activity,[50] although its affinity for the PR is greatly reduced relative to norethisterone at only 25% of that of progesterone.[3] Norethisterone produces similar changes in the endometrium and vagina, such as endometrial transformation, and is similarly antigonadotropic, ovulation-inhibiting, and thermogenic in women compared to progesterone, which is in accordance with its progestogenic activity.[51][49][52]

Androgenic activity edit

Norethisterone has approximately 15% of the affinity of the anabolic–androgenic steroid (AAS) metribolone (R-1881) for the AR, and in accordance, is weakly androgenic.[3] In contrast to norethisterone, 5α-DHNET, the major metabolite of norethisterone, shows higher affinity for the AR, with approximately 27% of the affinity of metribolone.[3] However, although 5α-DHNET has higher affinity for the AR than norethisterone, it has significantly diminished and in fact almost abolished androgenic potency in comparison to norethisterone in rodent bioassays.[53][54] Similar findings were observed for ethisterone (17α-ethynyltestosterone) and its 5α-reduced metabolite, whereas 5α-reduction enhanced both the AR affinity and androgenic potency of testosterone and nandrolone (19-nortestosterone) in rodent bioassays.[54] As such, it appears that the ethynyl group of norethisterone at the C17α position is responsible for its loss of androgenicity upon 5α-reduction.[54]

Norethisterone (0.5 to 3 mg/day) has been found to dose-dependently decrease circulating SHBG levels, which is a common property of androgens and is due to AR-mediated suppression of hepatic SHBG production.[38] The drug also has estrogenic activity, and estrogens are known to increase SHBG hepatic production and circulating levels, so it would appear that the androgenic activity of norethisterone overpowers its estrogenic activity in this regard.[38]

Norethisterone is bound to a considerable extent (36%) to SHBG in circulation.[3] Although it has lower affinity for SHBG than endogenous androgens and estrogens,[55] Norethisterone may displace testosterone from SHBG and thereby increase free testosterone levels, and this action may contribute to its weak androgenic effects.[56]

Estrogenic activity edit

 
Ethinylestradiol (EE), the metabolite of norethisterone responsible for its estrogenic activity.[3]

Norethisterone binds to the ERs, the ERα and the ERβ, with 0.07% and 0.01% of the relative binding affinity of estradiol.[57] Due to these very low relative affinities, it is essentially inactive itself as a ligand of the ERs at clinical concentrations.[3] However, norethisterone has been found to be a substrate for aromatase and is converted in the liver to a small extent (0.35%) to the highly potent estrogen ethinylestradiol (EE), and for this reason, unlike most other progestins, norethisterone has some estrogenic activity.[3] However, with typical dosages of norethisterone used in oral contraceptives (0.5 to 1 mg), the levels of EE produced are low, and it has been said that they are probably without clinical relevance.[3] Conversely, doses of 5 and 10 mg of norethisterone, which are used in the treatment of gynecological disorders, are converted at rates of 0.7% and 1.0% and produce levels of EE that correspond to those produced by 30 and 60 μg dosages of EE, respectively.[1][3] The levels of EE formed by 0.5 and 1 mg of norethisterone have been estimated based on higher dosages as corresponding to 2 and 10 μg dosages of EE, respectively.[1] At high doses, norethisterone may increase the risk of venous thromboembolism due to metabolism into EE.[58]

Neurosteroid activity edit

Like progesterone and testosterone, norethisterone is metabolized into 3,5-tetrahydro metabolites.[59] Whether these metabolites of norethisterone interact with the GABAA receptor similarly to the 3,5-tetrahydro metabolites of progesterone and testosterone like allopregnanolone and 3α-androstanediol, respectively, is a topic that does not appear to have been studied and hence requires clarification.[59]

Steroidogenesis inhibition edit

Norethisterone is a substrate for and is known to be an inhibitor of 5α-reductase, with 4.4% and 20.1% inhibition at 0.1 and 1 μM, respectively.[3] However, therapeutic concentrations of norethisterone are in the low nanomolar range, so this action may not be clinically relevant at typical dosages.[3]

Norethisterone and its major active metabolite 5α-DHNET have been found to act as irreversible aromatase inhibitors (Ki = 1.7 μM and 9.0 μM, respectively).[60] However, like the case of 5α-reductase, the concentrations required are probably too high to be clinically relevant at typical dosages.[3] 5α-DHNET specifically has been assessed and found to be selective in its inhibition of aromatase, and does not affect cholesterol side-chain cleavage enzyme (P450scc), 17α-hydroxylase/17,20-lyase, 21-hydroxylase, or 11β-hydroxylase.[60] Since it is not aromatized (and hence cannot be transformed into an estrogenic metabolite), unlike norethisterone, 5α-DHNET has been proposed as a potential therapeutic agent in the treatment of ER-positive breast cancer.[60]

Other activities edit

Norethisterone is a very weak inhibitor of CYP2C9 and CYP3A4 (IC50 = 46 μM and 51 μM, respectively), but these actions require very high concentrations of norethisterone that are far above therapeutic circulating levels (which are in the nanomolar range) and hence are probably not clinically relevant.[3]

Norethisterone and some of its 5α-reduced metabolites have been found to produce vasodilating effects in animals that are independent of sex steroid receptors and hence appear to be non-genomic in mechanism.[61]

Norethisterone stimulates the proliferation of MCF-7 breast cancer cells in vitro, an action that is independent of the classical PRs and is instead mediated via the progesterone receptor membrane component-1 (PGRMC1).[62] Certain other progestins act similarly in this assay, whereas progesterone acts neutrally.[62] It is unclear if these findings may explain the different risks of breast cancer observed with progesterone and progestins in clinical studies.[63]

Antigonadotropic effects edit

Due to its progestogenic activity, norethisterone suppresses the hypothalamic–pituitary–gonadal axis (HPG axis) and hence has antigonadotropic effects.[3][49] The estrogenic activity of norethisterone at high doses would also be expected to contribute to its antigonadotropic effects.[64] Due to its antigonadotropic effects, norethisterone suppresses gonadal sex hormone production, inhibits ovulation in women, and suppresses spermatogenesis in men.[3][49][65]

The ovulation-inhibiting dosage of both oral norethisterone and oral NETA is about 0.5 mg/day in women.[3][66][67] However, some conflicting data exist, suggesting that higher doses might be necessary for full inhibition of ovulation.[68] An intramuscular injection of 200 mg NETE has been found to prevent ovulation and suppress levels of estradiol, progesterone, luteinizing hormone (LH), and follicle-stimulating hormone (FSH) in women.[69][70][71][72]

Early studies of oral norethisterone in men employing doses of 20 to 50 mg/day observed suppression of 17-ketosteroid excretion, increased estrogen excretion (due to conversion into ethinylestradiol), suppression of spermatogenesis, libido, and erectile function, and incidence of gynecomastia.[73][74][75][44][76] A dosage of oral norethisterone of 25 mg/day for 3 weeks in men has been reported to suppress testosterone levels by about 70%, to 100 to 200 ng/dL, within 4 or 5 days, as well as to suppress sperm count and to have no effect on libido or erectile function over this short time period.[77][78] In healthy young men, NETA alone at a dose of 5 to 10 mg/day orally for 2 weeks suppressed testosterone levels from ~527 ng/dL to ~231 ng/dL (–56%).[79]

 
Hormone levels following a single intramuscular injection of estradiol valerate/norethisterone enanthate (5 mg/50 mg) (Mesigyna) in healthy young men.[80] Testosterone levels were maximally suppressed by about 94%, to ~30 ng/dL, when measured at day 7 post-injection.[80]

A single 200 mg intramuscular injection of NETE alone or in combination with 2 mg estradiol valerate has been found to produce a rapid, strong, and sustained decrease in gonadotropin and testosterone levels for up to one month in men.[65][81][82] Intramuscular injections of 200 mg NETE once every 3 weeks have also been found to suppress spermatogenesis in men.[73][83] Similarly, a single intramuscular injection of 50 mg NETE in combination with 5 mg estradiol valerate has been found to strongly suppress testosterone levels in men.[80] Levels of testosterone decreased from ~503 ng/dL at baseline to ~30 ng/dL at the lowest point (–94%) which occurred at day 7 post-injection.[80]

Pharmacokinetics edit

The pharmacokinetics of norethisterone have been reviewed.[3][84]

Absorption edit

The oral bioavailability of norethisterone is between 47 and 73%, with a mean oral bioavailability of 64%.[1][2] Micronization has been found to significantly improve the oral bioavailability of norethisterone by increasing intestinal absorption and reducing intestinal metabolism.[3][85] A single 2 mg oral dose of norethisterone has been found to result in peak circulating levels of the drug of 12 ng/mL (40 nmol/L), whereas a single 1 mg oral dose of norethisterone in combination with 2 mg estradiol resulted in peak levels of norethisterone of 8.5 ng/mL (29 nmol/L) one-hour post-administration.[3]

Hormone levels with norethisterone
  •  
    Norethisterone and ethinylestradiol levels over 24 hours after a single oral dose of 10 mg NETA in postmenopausal women.[38]
  •  
    Norethisterone and ethinylestradiol levels over 8 weeks after a single intramuscular injection of 200 mg NETE in premenopausal women.[86]

Distribution edit

The plasma protein binding of norethisterone is 97%.[3] It is bound 61% bound to albumin and 36% bound to SHBG.[3]

Metabolism edit

Metabolism of norethisterone and its prodrugs in humans
 
 
The metabolic pathways involved in the metabolism of norethisterone in humans. Norethisterone acetate, norethisterone enanthate, etynodiol, etynodiol diacetate, lynestrenol, noretynodrel, quingestanol, and quingestanol acetate are all prodrugs of norethisterone. Ethinylestradiol is an estrogenic metabolite of norethisterone formed by cytochrome P450 enzymes. The two isomers of dihydronorethisterone and the four isomers of tetrahydronorethisterone are formed by 5α- and 5β-reductases and 3α- and 3β-hydroxysteroid dehydrogenases and have diminished or absent activity. Norethisterone and its metabolites also undergo hydroxylation via cytochrome P450 enzymes and conjugation via glucuronidation and sulfation at available hydroxyl (–OH) groups. Sources:[87][88][89][90][91][92][7][49][3][93][94]

Norethisterone has an elimination half-life of 5.2 to 12.8 hours, with a mean elimination half-life of 8.0 hours.[1] The metabolism of norethisterone is very similar to that of testosterone (and nandrolone) and is mainly via reduction of the Δ4 double bond to 5α- and 5β-dihydronorethisterone, which is followed by the reduction of the C3 keto group to the four isomers of 3,5-tetrahydronorethisterone.[3] These transformations are catalyzed by 5α- and 5β-reductase and 3α- and 3β-hydroxysteroid dehydrogenase both in the liver and in extrahepatic tissues such as the pituitary gland, uterus, prostate gland, vagina, and breast.[95] With the exception of 3α,5α- and 3β,5α-tetrahydronorethisterone, which have significant affinity for the ER and are estrogenic to some degree, the 3,5-tetrahydro metabolites of norethisterone are inactive in terms of affinity for sex steroid receptors (specifically, the PR, AR, and ER).[96][97][98] A small amount of norethisterone is also converted by aromatase into EE.[1][3][45] Norethisterone is metabolized in the liver via hydroxylation as well, mainly by CYP3A4.[4] Some conjugation (including glucuronidation and sulfation)[95][99] of norethisterone and its metabolites occurs in spite of steric hindrance by the ethynyl group at C17α.[3] The ethynyl group of norethisterone is preserved in approximately 90% of all of its metabolites.[3]

Norethisterone is used in birth control pills, opposed to progesterone itself, because it is not metabolized as rapidly as progesterone when consumed orally. When progesterone is consumed orally it is rapidly metabolized in the gastrointestinal tract and the liver, and broken down into many different metabolites. Whereas, norethisterone is not as rapidly metabolized allowing norethisterone to be present in higher quantities allowing it to more effectively compete for progesterone receptor binding sites.[3]

Elimination edit

Norethisterone is eliminated 33 to 81% in urine and 35 to 43% in feces.[100]

Chemistry edit

See also: List of progestogens and List of androgens/anabolic steroids

Norethisterone, also known as 17α-ethynyl-19-nortestosterone or as 17α-ethynylestra-4-en-17β-ol-3-one, is a synthetic estrane steroid and a derivative of testosterone.[101][27] It is specifically a derivative of testosterone in which an ethynyl group has been added at the C17α position and the methyl group at the C19 position has been removed; hence, it is a combined derivative of ethisterone (17α-ethynyltestosterone) and nandrolone (19-nortestosterone).[101][27] These modifications result in increased progestogenic activity and oral bioavailability as well as decreased androgenic/anabolic activity.[102]

Derivatives edit

See also: Progestogen ester and List of progestogen esters

Norethisterone (NET) is the parent compound of a large group of progestins that includes most of the progestins known as the 19-nortestosterone derivatives.[103] This group is divided by chemical structure into the estranes (derivatives of norethisterone) and the gonanes (18-methylgonanes or 13β-ethylestranes; derivatives of levonorgestrel) and includes the following marketed medications:[104]

Several of these act as prodrugs of norethisterone, including NETA, NETE, etynodiol diacetate, lynestrenol, and quingestanol acetate.[105][106][107] Noretynodrel may also be a prodrug of norethisterone.[3][1] NETA is taken by mouth similarly to norethisterone, while NETE is given by injection into muscle.[10]

Non-17α-ethynylated edit

19-Nortestosterone (19-NT) progestins which are technically not derivatives of norethisterone (as they do not have a C17α ethynyl group) but are still closely related (with other substitutions at the C17α and/or C16β positions) include the following marketed medications:[101][27]

Many anabolic steroids of the 19-nortestosterone family, like norethandrolone and ethylestrenol, are also potent progestogens, but were never marketed as such.

Synthesis edit

Chemical syntheses of norethisterone have been published.[101][84]

Synthesis 1 edit

 
Norethisterone synthesis #1.[11][108]

Estradiol 3-methyl ether (1, EME) is partially reduced to the 1,5-diene (2) as also occurs for the first step in the synthesis of nandrolone. Oppenauer oxidation then transforms the C17β hydroxyl group into a ketone functionality (3). This is then reacted with metal acetylide into the corresponding C17α ethynyl compound (4). Hydrolysis of the enol ether under mild conditions leads directly to (5),[108] which appears to be noretynodrel (although Lednicer states that it is "etynodrel" in his book (which may be a synonym etynodiol); etynodrel is with a chlorine atom attached), an orally active progestin. This is the progestogen component of the first oral contraceptive to be offered for sale (i.e., Enovid). Treatment of the ethynyl enol ether with strong acid leads to norethisterone (6).[11]

In practice, these and all other combined oral contraceptives are mixtures of 1 to 2% EE or mestranol and an oral progestin. It has been speculated that the discovery of the necessity of estrogen in addition to progestin for contraceptive efficacy is due to the presence of a small amount of unreduced EME (1) in early batches of 2. This when subjected to oxidation and ethynylation, would of course lead to mestranol (3). In any event, the need for the presence of estrogen in the mixture is now well established experimentally.

Synthesis 2 edit

 
Norethisterone synthesis #2.[109][110][111][112][113]

Norethisterone is made from estr-4-ene-3,17-dione (bolandione), which in turn is synthesized by partial reduction of the aromatic region of the 3-O-methyl ether of estrone with lithium in liquid ammonia, and simultaneously of the keto group at C17α to a hydroxyl group, which is then oxidized back to a keto group by chromium trioxide in acetic acid. The conjugated C4-C5 olefin and the carbonyl group at C3 is then transformed to dienol ethyl ether using ethyl orthoformate. The obtained product is ethynylated by acetylene in the presence of potassium tert-butoxide. After hydrochloride hydrolysis of the formed O-potassium derivative, during which the enol ether is also hydrolyzed, and the remaining double bond is shifted, the desired norethisterone is obtained.

History edit

Norethisterone was synthesized for the first time by chemists Luis Miramontes, Carl Djerassi, and George Rosenkranz at Syntex in Mexico City in 1951.[11] It was derived from ethisterone, and was found to possess about 20-fold greater potency as a progestogen in comparison.[citation needed] Norethisterone was the first highly active oral progestogen to be synthesized, and was preceded (as a progestogen) by progesterone (1934), ethisterone (1938), 19-norprogesterone (1944), and 17α-methylprogesterone (1949) as well as by nandrolone (1950), whereas noretynodrel (1952) and norethandrolone (1953) followed the synthesis of norethisterone.[12][13] The drug was introduced as Norlutin in the United States in 1957.[14] Norethisterone was subsequently combined with mestranol and marketed as Ortho-Novum in the United States in 1963. It was the second progestin, after noretynodrel in 1960, to be used in an oral contraceptive.[13] In 1964, additional contraceptive preparations containing norethisterone in combination with mestranol or EE, such as Norlestrin and Norinyl, were marketed in the United States.[13]

Society and culture edit

Generic names edit

Norethisterone is the INNTooltip International Nonproprietary Name and BANTooltip British Approved Name of the drug while norethindrone is its USANTooltip United States Adopted Name.[101][27]

Brand names edit

Norethisterone is available in Bangladesh as Menogia (ACI), Normens (Renata) etc. Norethisterone (NET), including as NETA and NETE, has been marketed under many brand names throughout the world.[27][19]

Availability edit

United States edit

See also: List of progestogens available in the United States

Norethisterone was previously available alone in 5 mg tablets under the brand names Norlutin in the United States, but this formulation has since been discontinued in this country.[26] However, NETA remains available alone in 5 mg tablets under the brand name Aygestin in the United States.[26] It is one of the only non-contraceptive progestogen-only drug formulations that remains available in the United States.[26] The others include progesterone, medroxyprogesterone acetate, megestrol acetate, and hydroxyprogesterone caproate, as well as the atypical agent danazol.[26]

Both norethisterone and NETA are also available in the United States as contraceptives.[26] Norethisterone is available both alone (brand names Camila, Errin, Heather, Micronor, Nor-QD, others) and in combination with EE (Norinyl, Ortho-Novum, others) or mestranol (Norinyl, Ortho-Novum, others), while NETA is available only in combination with EE (Norlestrin, others).[26] NETE is not available in the United States in any form.[26][114][115]

Research edit

Norethisterone, as NETA and NETE, has been studied for use as a potential male hormonal contraceptive in combination with testosterone in men.[116][117]

Long-acting norethisterone microspheres for intramuscular injection have been studied for potential use in birth control.[118]

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Further reading edit

  • Brogden RN, Speight TM, Avery GS (1973). "Progestagen-only oral contraceptives: a preliminary report of the action and clinical use of norgestrel and norethisterone". Drugs. 6 (3): 169–81. doi:10.2165/00003495-197306030-00004. PMID 4130566. S2CID 42295736.
  • "Norethisterone and norethisterone acetate". IARC Monographs on the Evaluation of the Carcinogenic Risk of Chemicals to Humans. 21: 441–60. December 1979. PMID 120838.
  • Stanczyk FZ, Roy S (July 1990). "Metabolism of levonorgestrel, norethindrone, and structurally related contraceptive steroids". Contraception. 42 (1): 67–96. doi:10.1016/0010-7824(90)90093-b. PMID 2143719.
  • Wiseman LR, McTavish D (March 1994). "Transdermal estradiol/norethisterone. A review of its pharmacological properties and clinical use in postmenopausal women". Drugs & Aging. 4 (3): 238–56. doi:10.2165/00002512-199404030-00006. PMID 8199397. S2CID 68007924.
  • Taitel HF, Kafrissen ME (1995). "Norethindrone--a review of therapeutic applications". International Journal of Fertility and Menopausal Studies. 40 (4): 207–23. PMID 8520623.
  • Maier WE, Herman JR (August 2001). "Pharmacology and toxicology of ethinyl estradiol and norethindrone acetate in experimental animals". Regulatory Toxicology and Pharmacology. 34 (1): 53–61. doi:10.1006/rtph.2001.1483. PMID 11502156.
  • Riis BJ, Lehmann HJ, Christiansen C (October 2002). "Norethisterone acetate in combination with estrogen: effects on the skeleton and other organs. A review". American Journal of Obstetrics and Gynecology. 187 (4): 1101–16. doi:10.1067/mob.2002.122852. PMID 12389012.
  • Draper BH, Morroni C, Hoffman M, Smit J, Beksinska M, Hapgood J, Van der Merwe L (July 2006). "Depot medroxyprogesterone versus norethisterone oenanthate for long-acting progestogenic contraception". The Cochrane Database of Systematic Reviews (3): CD005214. doi:10.1002/14651858.CD005214.pub2. PMID 16856087.
  • Kuhl H, Wiegratz I (August 2007). "Can 19-nortestosterone derivatives be aromatized in the liver of adult humans? Are there clinical implications?". Climacteric. 10 (4): 344–53. doi:10.1080/13697130701380434. PMID 17653961. S2CID 20759583.
  • Casey CL, Murray CA (2008). "HT update: spotlight on estradiol/norethindrone acetate combination therapy". Clinical Interventions in Aging. 3 (1): 9–16. doi:10.2147/cia.s1663. PMC 2544373. PMID 18488874.
  • Paulen ME, Curtis KM (October 2009). "When can a woman have repeat progestogen-only injectables--depot medroxyprogesterone acetate or norethisterone enantate?". Contraception. 80 (4): 391–408. doi:10.1016/j.contraception.2009.03.023. PMID 19751863.
  • Chwalisz K, Surrey E, Stanczyk FZ (June 2012). "The hormonal profile of norethindrone acetate: rationale for add-back therapy with gonadotropin-releasing hormone agonists in women with endometriosis". Reproductive Sciences. 19 (6): 563–71. doi:10.1177/1933719112438061. PMID 22457429. S2CID 2882899.

January 01, 1970
norethisterone, also, known, norethindrone, sold, under, many, brand, names, progestin, medication, used, birth, control, pills, menopausal, hormone, therapy, treatment, gynecological, disorders, medication, available, both, dose, high, dose, formulations, bot. Norethisterone also known as norethindrone and sold under many brand names is a progestin medication used in birth control pills menopausal hormone therapy and for the treatment of gynecological disorders 3 5 The medication is available in both low dose and high dose formulations and both alone and in combination with an estrogen 5 6 It is used by mouth or as norethisterone enanthate by injection into muscle 3 5 7 NorethisteroneClinical dataTrade namesManyOther namesNET Norethindrone NSC 9564 LG 202 Ethinylnortestosterone Norpregneninolone Anhydrohydroxy norprogesterone Ethinylestrenolone 17a Ethynyl 19 nortestosterone 17a Ethynylestra 4 en 17b ol 3 one 17a Hydroxy 19 norpregn 4 en 20 yn 3 oneAHFS Drugs comMonographMedlinePlusa604034License dataUS DailyMed NorethindroneRoutes ofadministrationBy mouth intramuscular injection as NETETooltip norethisterone enanthate Drug classProgestogen medication ProgestinATC codeG03AC01 WHO G03DC02 WHO Legal statusLegal statusUS onlyPharmacokinetic dataBioavailability47 73 mean 64 1 2 Protein binding97 3 Albumin 61 3 SHBGTooltip Sex hormone binding globulin 36 3 MetabolismMainly CYP3A4 liver 4 also 5a 5b reductase 3a Tooltip 3a hydroxysteroid dehydrogenase 3b HSDTooltip 3b hydroxysteroid dehydrogenase and aromataseElimination half life5 2 12 8 hours mean 8 0 hours 1 IdentifiersIUPAC name 8R 9S 10R 13S 14S 17R 17 ethynyl 17 hydroxy 13 methyl 1 2 6 7 8 9 10 11 12 14 15 16 dodecahydrocyclopenta a phenanthren 3 oneCAS Number68 22 4 YPubChem CID6230IUPHAR BPS2880DrugBankDB00717 YChemSpider5994 YUNIIT18F433X4SKEGGD00182 YChEBICHEBI 7627 YChEMBLChEMBL1162 YCompTox Dashboard EPA DTXSID9023380ECHA InfoCard100 000 619Chemical and physical dataFormulaC 20H 26O 2Molar mass298 426 g mol 13D model JSmol Interactive imageMelting point203 to 204 C 397 to 399 F SMILES C C 12CC C H 3 C H C H 1CC C 2 C C O CCC4 CC O CC C H 34InChI InChI 1S C20H26O2 c1 3 20 22 11 9 18 17 6 4 13 12 14 21 5 7 15 13 16 17 8 10 19 18 20 2 h1 12 15 18 22H 4 11H2 2H3 t15 16 17 18 19 20 m0 s1 YKey VIKNJXKGJWUCNN XGXHKTLJSA N Y verify Side effects of norethisterone include menstrual irregularities headaches nausea breast tenderness mood changes acne increased hair growth 8 9 Norethisterone is a progestin or a synthetic progestogen and hence is an agonist of the progesterone receptor the biological target of progestogens like progesterone 3 5 It has weak androgenic and estrogenic activity mostly at high dosages and no other important hormonal activity 3 10 Norethisterone was discovered in 1951 and was one of the first progestins to be developed 11 12 13 It was first introduced for medical use on its own in 1957 and was introduced in combination with an estrogen for use as a birth control pill in 1963 13 14 It is sometimes referred to as a first generation progestin 15 16 Along with desogestrel it is one of the only progestins that is widely available as a progestogen only mini pill for birth control 17 18 Norethisterone is marketed widely throughout the world 19 It is available as a generic medication 20 In 2021 it was the 140th most commonly prescribed medication in the United States with more than 4 million prescriptions 21 22 It is on the World Health Organization s List of Essential Medicines 23 Contents 1 Medical uses 2 Contraindications 3 Side effects 3 1 Androgenic 3 2 Estrogenic 4 Overdose 5 Interactions 6 Pharmacology 6 1 Pharmacodynamics 6 1 1 Progestogenic activity 6 1 2 Androgenic activity 6 1 3 Estrogenic activity 6 1 4 Neurosteroid activity 6 1 5 Steroidogenesis inhibition 6 1 6 Other activities 6 1 7 Antigonadotropic effects 6 2 Pharmacokinetics 6 2 1 Absorption 6 2 2 Distribution 6 2 3 Metabolism 6 2 4 Elimination 7 Chemistry 7 1 Derivatives 7 1 1 Non 17a ethynylated 7 2 Synthesis 7 2 1 Synthesis 1 7 2 2 Synthesis 2 8 History 9 Society and culture 9 1 Generic names 9 2 Brand names 9 3 Availability 9 3 1 United States 10 Research 11 References 12 Further readingMedical uses editNorethisterone is used as a hormonal contraceptive in combination with an estrogen usually ethinylestradiol EE in combined oral contraceptive pills and alone in progestogen only pills Another medical use of norethisterone is to alleviate endometriosis related pain In fact 50 of patients who received medical or surgical treatment for endometriosis related pelvic pain have benefited from progestin therapy This could be due to the fact that norethisterone induces endometrial proliferation during secretory phase which has been shown to alleviate endometrial pain complaints Another way in which norethisterone may be acting to reduce endometrial pain is via inhibition of ovulation Endometriosis pain and discomfort is worse during ovulation 24 vte Formulations and brand names of norethisterone and esters Composition Dose Brand names Use NET only Low e g 0 35 mg Multiple a Progestogen only oral contraceptive NET or NETA only High e g 5 mg 10 mg Multiple b Gynecological disorders and other uses NETE only Injection e g 200 mg Multiple c Progestogen only injectable contraceptive NET or NETA with ethinylestradiol Low e g 0 4 mg 0 5 mg 0 75 mg 1 mg 1 5 mg Multiple d Combined oral contraceptive NET with mestranol Low e g 1 mg 2 mg Multiple e Combined oral contraceptive NETA with estradiol Low e g 0 1 mg 0 5 mg Multiple f Combined menopausal hormone therapy NETE with estradiol valerate Injection e g 50 mg Multiple g Combined injectable contraceptive Abbreviations NET Norethisterone NETA Norethisterone acetate NETE Norethisterone enanthate Sources 25 26 27 28 Notes Camila Errin Heather Jencycla Jolivette Locilan Micro Novum Micronovum Micronor Nor QD Nora Noriday Ortho Micronor Aygestin Lupaneta Pack combination pack with leuprorelin Norcolut Norlutate Primolut N Primolut Nor SH 420 Utovlan Depocon Doryxas NET EN Noristerat Norigest Nur Isterate Aranelle Balziva Binovum Brevicon Brevinor Briellyn Cyclafem Dasetta Estrostep Femcon Generess Gildagia Gildess Jinteli Junel Larin Leena Lo Loestrin Lo Minastrin Loestrin Lolo Lomedia Microgestin Minastrin Modicon Nelova Norimin Norinyl Nortrel Ortho Ortho Novum Ovcon Ovysmen Philith Primella Select Synphase Synphasic Tilia Tri Legest Tri Norinyl Trinovum Vyfemla Wera Wymzya Zenchent Zeosa Norethin Noriday Norinyl Norquen Ortho Novum Sophia Activella Activelle Alyacen Cliane Climagest Climesse Cliovelle CombiPatch Elleste Duet Estalis Estropause Eviana Evorel Kliane Kliofem Kliogest Kliovance Mesigyna Mesygest Mimvey Necon Novofem Nuvelle Sequidot Systen Trisequens Chinese Injectable No 3 Efectimes Ginediol Mesigyna Mesilar Meslart Mesocept Mesygest Nofertyl Nofertyl Lafrancol Noregyna Norestrin Norifam Norigynon Nostidyn Sexseg SolounaContraindications editHigh dose 10 mg day norethisterone has been associated with hepatic veno occlusive disease and because of this adverse effect norethisterone should not be given to patients undergoing allogeneic bone marrow transplantation as it has been associated with substantially lower one year survival post transplantation 29 217 30 Side effects editAt contraceptive and hormone replacement dosages 0 35 to 1 mg day norethisterone has essentially progestogenic side effects only In most clinical studies of norethisterone for contraception or menopausal hormone therapy the drug has been combined with an estrogen and for this reason it is difficult to determine which of the side effects were caused by norethisterone and which of them were caused by estrogen in such research However NETE an intramuscularly administered prodrug of norethisterone which is used as a long acting contraceptive is used without an estrogen and hence can be employed as a surrogate for norethisterone in terms of understanding its effects and tolerability In clinical studies the most common side effect with NETE has been menstrual disturbances including prolonged bleeding or spotting and amenorrhea 29 253 Other side effects have included periodic abdominal bloating and breast tenderness both of which are thought to be due to water retention and can be relieved with diuretics 29 253 There has been no association with weight gain and blood pressure blood clotting and glucose tolerance have all remained normal 29 253 However a decrease in HDL cholesterol has been observed 29 253 At high doses 5 to 60 mg day for instance those used in the treatment of gynecological disorders norethisterone can cause hypogonadism due to its antigonadotropic effects and can have estrogenic and weak androgenic side effects High doses of NETA 10 mg day have been associated with abnormal liver function tests including significant elevations in liver enzymes 31 32 33 These liver enzymes included lactate dehydrogenase and glutamate pyruvate transaminase 33 Although they were described as having no clinical relevance 33 the elevated liver enzymes associated with NETA may have precluded its further development for male hormonal contraception 31 32 Androgenic edit Due to its weak androgenic activity norethisterone can produce androgenic side effects such as acne hirsutism and voice changes of slight severity in some women at high dosages e g 10 to 40 mg day 9 This is notably not the case with combined oral contraceptives that contain norethisterone and EE however 10 Such formulations contain low dosages of norethisterone 0 35 to 1 mg day 10 in combination with estrogen and are actually associated with improvement in acne symptoms 34 35 In accordance they are in fact approved by the FDATooltip Food and Drug Administration for the treatment of acne in women in the United States 34 35 The improvement in acne symptoms is believed to be due to a 2 to 3 fold increase in sex hormone binding globulin SHBG levels and a consequent decrease in free testosterone levels caused by EE which results in an overall decrease in androgenic signaling in the body 36 The sebaceous glands are highly androgen sensitive and their size and activity are potential markers of androgenic effect 37 A high dosage of 20 mg day norethisterone or NETA has been found to significantly stimulate the sebaceous glands whereas lower dosages of 5 mg day and 2 5 mg day norethisterone and NETA respectively did not significantly stimulate sebum production and were consequently regarded as devoid of significant androgenicity 37 Conversely dosages of norethisterone of 0 5 to 3 mg day have been found to dose dependently decrease SHBG levels and hence to suppress hepatic SHBG production which is another highly sensitive marker of androgenicity 38 A large clinical study of high to very high oral dosages of norethisterone 10 to 40 mg day administered for prolonged periods of time 4 to 35 weeks to prevent miscarriage in pregnant women found that 5 5 of the women experienced mild androgenic side effects such as mild voice changes hoarseness acne and hirsutism and that 18 3 of female infants born to the mothers showed in most cases only slight virilization of the genitals 9 Maternal androgenic symptoms occurred most often in women who received a dosage of norethisterone of 30 mg day or more for a period of 15 weeks or longer 9 In the female infants who experienced virilization of the genitals the sole manifestation in 86 7 of the cases was varied but almost always slight enlargement of the clitoris 9 In the remaining 13 3 of the affected cases marked clitoral enlargement and partial fusion of the labioscrotal folds occurred 9 The dosages used in these cases were 20 to 40 mg day 9 In a letter to the editor on the topic of virilization caused by high dosages of NETA in women a physician expressed that they had not observed the slightest evidence of virilization and that there had certainly been no hirsutism nor any voice changes in 55 women with advanced breast cancer that they had treated with 30 to 60 mg day norethisterone for up to six months 39 High dosage norethisterone has been used to suppress menstruation in women with severe intellectual disability who were incapable of handling their own menses 40 41 A study of 118 nulliparous women treated with 5 mg day norethisterone for a period of 2 to 30 months found that the drug was effective in producing amenorrhea in 86 of the women with breakthrough bleeding occurring in the remaining 14 40 Side effects including weight gain hirsutism acne headache nausea and vomiting all did not appear to increase in incidence and no disturbing side effects were noted in any of the women 40 41 Another study of 5 mg day norethisterone in 132 women also made no mention of androgenic side effects 42 These findings suggest little to no risk of androgenic side effects with norethisterone at a dosage of 5 mg day 40 41 A study of 194 women treated with 5 to 15 mg day NETA for a median duration of 13 months of therapy to suppress symptoms of endometriosis observed no side effects in 55 2 of patients weight gain in 16 1 acne in 9 9 mood lability in 8 9 hot flashes in 8 3 and voice deepening in two women 1 0 43 Estrogenic edit Norethisterone is weakly estrogenic via conversion into its metabolite EE and for this reason it has been found at high dosages to be associated with high rates of estrogenic side effects such as breast enlargement in women and gynecomastia in men but also with improvement of menopausal symptoms in postmenopausal women 44 It has been suggested that very high dosages e g 40 mg day which are sometimes used in clinical practice for various indications of NETA and by extension norethisterone may result in an increased risk of venous thromboembolism VTE analogously to high dosages above 50 mg day of EE and that even doses of NETA of 10 to 20 mg which correspond to EE doses of approximately 20 to 30 mg day may in certain women be associated with increased risk 45 46 A study also found that ethinylestradiol and norethisterone had a greater influence on coagulation factors when the dose of norethisterone was 3 or 4 mg than when it was 1 mg 47 This might have been due to additional ethinylestradiol generated by higher doses of norethisterone 47 Overdose editThere have been no reports of serious side effects with overdose of norethisterone even in small children 48 As such overdose usually does not require treatment 48 High dosages of as much as 60 mg day norethisterone have been studied for extended treatment durations without serious adverse effects described 39 Interactions edit5a Reductase plays an important role in the metabolism of norethisterone and 5a reductase inhibitors such as finasteride and dutasteride can inhibit its metabolism citation needed Norethisterone is partially metabolized via hydroxylation by CYP3A4 and inhibitors and inducers of CYP3A4 can significantly alter circulating levels of norethisterone 4 For instance the CYP3A4 inducers rifampicin and bosentan have been found to decrease norethisterone exposure by 42 and 23 respectively and the CYP3A4 inducers carbamazepine and St John s wort have also been found to accelerate norethisterone clearance 4 Pharmacology editPharmacodynamics edit Norethisterone is a potent progestogen and a weak androgen and estrogen 3 That is it is a potent agonist of the progesterone receptor PR and a weak agonist of the androgen receptor AR and the estrogen receptor ER 3 Norethisterone itself has insignificant affinity for the ER its estrogenic activity is from an active metabolite that is formed in very small amounts ethinylestradiol EE which is a very potent estrogen 3 Norethisterone and its metabolites have negligible affinity for the glucocorticoid receptor GR and mineralocorticoid receptor MR and hence have no glucocorticoid antiglucocorticoid mineralocorticoid or antimineralocorticoid activity 3 vte Relative affinities of norethisterone metabolites and prodrugs Compound Typea PRTooltip Progesterone receptor ARTooltip Androgen receptor ERTooltip Estrogen receptor GRTooltip Glucocorticoid receptor MRTooltip Mineralocorticoid receptor SHBGTooltip Sex hormone binding globulin CBGTooltip Corticosteroid binding globulin Norethisterone 67 75 15 0 0 1 0 3 16 0 5a Dihydronorethisterone Metabolite 25 27 0 0 3a 5a Tetrahydronorethisterone Metabolite 1 0 0 1 0 3a 5b Tetrahydronorethisterone Metabolite 0 0 3b 5a Tetrahydronorethisterone Metabolite 1 0 0 8 0 Ethinylestradiol Metabolite 15 25 1 3 112 1 3 0 0 18 0 Norethisterone acetate Prodrug 20 5 1 0 0 Norethisterone enanthate Prodrug Noretynodrel Prodrug 6 0 2 0 0 0 0 Etynodiol Prodrug 1 0 11 18 0 Etynodiol diacetate Prodrug 1 0 0 0 0 Lynestrenol Prodrug 1 1 3 0 0 Notes Values are percentages Reference ligands 100 were promegestone for the PRTooltip progesterone receptor metribolone for the ARTooltip androgen receptor estradiol for the ERTooltip estrogen receptor dexamethasone for the GRTooltip glucocorticoid receptor aldosterone for the MRTooltip mineralocorticoid receptor dihydrotestosterone for SHBGTooltip sex hormone binding globulin and cortisol for CBGTooltip Corticosteroid binding globulin Footnotes a Active or inactive metabolite prodrug or neither of norethisterone Sources See template Progestogenic activity edit Norethisterone is a potent progestogen and binds to the PR with approximately 150 of the affinity of progesterone 3 In contrast its parent compounds testosterone nandrolone 19 nortestosterone and ethisterone 17a ethynyltestosterone have 2 22 and 44 of the relative binding affinity of progesterone for the PR 49 Unlike norethisterone its major active metabolite 5a dihydronorethisterone 5a DHNET which is formed by transformation via 5a reductase has been found to possess both progestogenic and marked antiprogestogenic activity 50 although its affinity for the PR is greatly reduced relative to norethisterone at only 25 of that of progesterone 3 Norethisterone produces similar changes in the endometrium and vagina such as endometrial transformation and is similarly antigonadotropic ovulation inhibiting and thermogenic in women compared to progesterone which is in accordance with its progestogenic activity 51 49 52 Androgenic activity edit Norethisterone has approximately 15 of the affinity of the anabolic androgenic steroid AAS metribolone R 1881 for the AR and in accordance is weakly androgenic 3 In contrast to norethisterone 5a DHNET the major metabolite of norethisterone shows higher affinity for the AR with approximately 27 of the affinity of metribolone 3 However although 5a DHNET has higher affinity for the AR than norethisterone it has significantly diminished and in fact almost abolished androgenic potency in comparison to norethisterone in rodent bioassays 53 54 Similar findings were observed for ethisterone 17a ethynyltestosterone and its 5a reduced metabolite whereas 5a reduction enhanced both the AR affinity and androgenic potency of testosterone and nandrolone 19 nortestosterone in rodent bioassays 54 As such it appears that the ethynyl group of norethisterone at the C17a position is responsible for its loss of androgenicity upon 5a reduction 54 Norethisterone 0 5 to 3 mg day has been found to dose dependently decrease circulating SHBG levels which is a common property of androgens and is due to AR mediated suppression of hepatic SHBG production 38 The drug also has estrogenic activity and estrogens are known to increase SHBG hepatic production and circulating levels so it would appear that the androgenic activity of norethisterone overpowers its estrogenic activity in this regard 38 Norethisterone is bound to a considerable extent 36 to SHBG in circulation 3 Although it has lower affinity for SHBG than endogenous androgens and estrogens 55 Norethisterone may displace testosterone from SHBG and thereby increase free testosterone levels and this action may contribute to its weak androgenic effects 56 Estrogenic activity edit nbsp Ethinylestradiol EE the metabolite of norethisterone responsible for its estrogenic activity 3 Norethisterone binds to the ERs the ERa and the ERb with 0 07 and 0 01 of the relative binding affinity of estradiol 57 Due to these very low relative affinities it is essentially inactive itself as a ligand of the ERs at clinical concentrations 3 However norethisterone has been found to be a substrate for aromatase and is converted in the liver to a small extent 0 35 to the highly potent estrogen ethinylestradiol EE and for this reason unlike most other progestins norethisterone has some estrogenic activity 3 However with typical dosages of norethisterone used in oral contraceptives 0 5 to 1 mg the levels of EE produced are low and it has been said that they are probably without clinical relevance 3 Conversely doses of 5 and 10 mg of norethisterone which are used in the treatment of gynecological disorders are converted at rates of 0 7 and 1 0 and produce levels of EE that correspond to those produced by 30 and 60 mg dosages of EE respectively 1 3 The levels of EE formed by 0 5 and 1 mg of norethisterone have been estimated based on higher dosages as corresponding to 2 and 10 mg dosages of EE respectively 1 At high doses norethisterone may increase the risk of venous thromboembolism due to metabolism into EE 58 Neurosteroid activity edit Like progesterone and testosterone norethisterone is metabolized into 3 5 tetrahydro metabolites 59 Whether these metabolites of norethisterone interact with the GABAA receptor similarly to the 3 5 tetrahydro metabolites of progesterone and testosterone like allopregnanolone and 3a androstanediol respectively is a topic that does not appear to have been studied and hence requires clarification 59 Steroidogenesis inhibition edit Norethisterone is a substrate for and is known to be an inhibitor of 5a reductase with 4 4 and 20 1 inhibition at 0 1 and 1 mM respectively 3 However therapeutic concentrations of norethisterone are in the low nanomolar range so this action may not be clinically relevant at typical dosages 3 Norethisterone and its major active metabolite 5a DHNET have been found to act as irreversible aromatase inhibitors Ki 1 7 mM and 9 0 mM respectively 60 However like the case of 5a reductase the concentrations required are probably too high to be clinically relevant at typical dosages 3 5a DHNET specifically has been assessed and found to be selective in its inhibition of aromatase and does not affect cholesterol side chain cleavage enzyme P450scc 17a hydroxylase 17 20 lyase 21 hydroxylase or 11b hydroxylase 60 Since it is not aromatized and hence cannot be transformed into an estrogenic metabolite unlike norethisterone 5a DHNET has been proposed as a potential therapeutic agent in the treatment of ER positive breast cancer 60 Other activities edit Norethisterone is a very weak inhibitor of CYP2C9 and CYP3A4 IC50 46 mM and 51 mM respectively but these actions require very high concentrations of norethisterone that are far above therapeutic circulating levels which are in the nanomolar range and hence are probably not clinically relevant 3 Norethisterone and some of its 5a reduced metabolites have been found to produce vasodilating effects in animals that are independent of sex steroid receptors and hence appear to be non genomic in mechanism 61 Norethisterone stimulates the proliferation of MCF 7 breast cancer cells in vitro an action that is independent of the classical PRs and is instead mediated via the progesterone receptor membrane component 1 PGRMC1 62 Certain other progestins act similarly in this assay whereas progesterone acts neutrally 62 It is unclear if these findings may explain the different risks of breast cancer observed with progesterone and progestins in clinical studies 63 Antigonadotropic effects edit Due to its progestogenic activity norethisterone suppresses the hypothalamic pituitary gonadal axis HPG axis and hence has antigonadotropic effects 3 49 The estrogenic activity of norethisterone at high doses would also be expected to contribute to its antigonadotropic effects 64 Due to its antigonadotropic effects norethisterone suppresses gonadal sex hormone production inhibits ovulation in women and suppresses spermatogenesis in men 3 49 65 The ovulation inhibiting dosage of both oral norethisterone and oral NETA is about 0 5 mg day in women 3 66 67 However some conflicting data exist suggesting that higher doses might be necessary for full inhibition of ovulation 68 An intramuscular injection of 200 mg NETE has been found to prevent ovulation and suppress levels of estradiol progesterone luteinizing hormone LH and follicle stimulating hormone FSH in women 69 70 71 72 Early studies of oral norethisterone in men employing doses of 20 to 50 mg day observed suppression of 17 ketosteroid excretion increased estrogen excretion due to conversion into ethinylestradiol suppression of spermatogenesis libido and erectile function and incidence of gynecomastia 73 74 75 44 76 A dosage of oral norethisterone of 25 mg day for 3 weeks in men has been reported to suppress testosterone levels by about 70 to 100 to 200 ng dL within 4 or 5 days as well as to suppress sperm count and to have no effect on libido or erectile function over this short time period 77 78 In healthy young men NETA alone at a dose of 5 to 10 mg day orally for 2 weeks suppressed testosterone levels from 527 ng dL to 231 ng dL 56 79 nbsp Hormone levels following a single intramuscular injection of estradiol valerate norethisterone enanthate 5 mg 50 mg Mesigyna in healthy young men 80 Testosterone levels were maximally suppressed by about 94 to 30 ng dL when measured at day 7 post injection 80 A single 200 mg intramuscular injection of NETE alone or in combination with 2 mg estradiol valerate has been found to produce a rapid strong and sustained decrease in gonadotropin and testosterone levels for up to one month in men 65 81 82 Intramuscular injections of 200 mg NETE once every 3 weeks have also been found to suppress spermatogenesis in men 73 83 Similarly a single intramuscular injection of 50 mg NETE in combination with 5 mg estradiol valerate has been found to strongly suppress testosterone levels in men 80 Levels of testosterone decreased from 503 ng dL at baseline to 30 ng dL at the lowest point 94 which occurred at day 7 post injection 80 Pharmacokinetics edit The pharmacokinetics of norethisterone have been reviewed 3 84 Absorption edit The oral bioavailability of norethisterone is between 47 and 73 with a mean oral bioavailability of 64 1 2 Micronization has been found to significantly improve the oral bioavailability of norethisterone by increasing intestinal absorption and reducing intestinal metabolism 3 85 A single 2 mg oral dose of norethisterone has been found to result in peak circulating levels of the drug of 12 ng mL 40 nmol L whereas a single 1 mg oral dose of norethisterone in combination with 2 mg estradiol resulted in peak levels of norethisterone of 8 5 ng mL 29 nmol L one hour post administration 3 Hormone levels with norethisterone nbsp Norethisterone and ethinylestradiol levels over 24 hours after a single oral dose of 10 mg NETA in postmenopausal women 38 nbsp Norethisterone and ethinylestradiol levels over 8 weeks after a single intramuscular injection of 200 mg NETE in premenopausal women 86 Distribution edit The plasma protein binding of norethisterone is 97 3 It is bound 61 bound to albumin and 36 bound to SHBG 3 Metabolism edit Metabolism of norethisterone and its prodrugs in humans nbsp nbsp The metabolic pathways involved in the metabolism of norethisterone in humans Norethisterone acetate norethisterone enanthate etynodiol etynodiol diacetate lynestrenol noretynodrel quingestanol and quingestanol acetate are all prodrugs of norethisterone Ethinylestradiol is an estrogenic metabolite of norethisterone formed by cytochrome P450 enzymes The two isomers of dihydronorethisterone and the four isomers of tetrahydronorethisterone are formed by 5a and 5b reductases and 3a and 3b hydroxysteroid dehydrogenases and have diminished or absent activity Norethisterone and its metabolites also undergo hydroxylation via cytochrome P450 enzymes and conjugation via glucuronidation and sulfation at available hydroxyl OH groups Sources 87 88 89 90 91 92 7 49 3 93 94 Norethisterone has an elimination half life of 5 2 to 12 8 hours with a mean elimination half life of 8 0 hours 1 The metabolism of norethisterone is very similar to that of testosterone and nandrolone and is mainly via reduction of the D4 double bond to 5a and 5b dihydronorethisterone which is followed by the reduction of the C3 keto group to the four isomers of 3 5 tetrahydronorethisterone 3 These transformations are catalyzed by 5a and 5b reductase and 3a and 3b hydroxysteroid dehydrogenase both in the liver and in extrahepatic tissues such as the pituitary gland uterus prostate gland vagina and breast 95 With the exception of 3a 5a and 3b 5a tetrahydronorethisterone which have significant affinity for the ER and are estrogenic to some degree the 3 5 tetrahydro metabolites of norethisterone are inactive in terms of affinity for sex steroid receptors specifically the PR AR and ER 96 97 98 A small amount of norethisterone is also converted by aromatase into EE 1 3 45 Norethisterone is metabolized in the liver via hydroxylation as well mainly by CYP3A4 4 Some conjugation including glucuronidation and sulfation 95 99 of norethisterone and its metabolites occurs in spite of steric hindrance by the ethynyl group at C17a 3 The ethynyl group of norethisterone is preserved in approximately 90 of all of its metabolites 3 Norethisterone is used in birth control pills opposed to progesterone itself because it is not metabolized as rapidly as progesterone when consumed orally When progesterone is consumed orally it is rapidly metabolized in the gastrointestinal tract and the liver and broken down into many different metabolites Whereas norethisterone is not as rapidly metabolized allowing norethisterone to be present in higher quantities allowing it to more effectively compete for progesterone receptor binding sites 3 Elimination edit Norethisterone is eliminated 33 to 81 in urine and 35 to 43 in feces 100 Chemistry editSee also List of progestogens and List of androgens anabolic steroids Norethisterone also known as 17a ethynyl 19 nortestosterone or as 17a ethynylestra 4 en 17b ol 3 one is a synthetic estrane steroid and a derivative of testosterone 101 27 It is specifically a derivative of testosterone in which an ethynyl group has been added at the C17a position and the methyl group at the C19 position has been removed hence it is a combined derivative of ethisterone 17a ethynyltestosterone and nandrolone 19 nortestosterone 101 27 These modifications result in increased progestogenic activity and oral bioavailability as well as decreased androgenic anabolic activity 102 Derivatives edit See also Progestogen ester and List of progestogen esters Norethisterone NET is the parent compound of a large group of progestins that includes most of the progestins known as the 19 nortestosterone derivatives 103 This group is divided by chemical structure into the estranes derivatives of norethisterone and the gonanes 18 methylgonanes or 13b ethylestranes derivatives of levonorgestrel and includes the following marketed medications 104 Estranes Etynodiol diacetate 3b hydroxy NET 3b 17b diacetate Lynestrenol 3 desoxy NET Norethisterone acetate NET 17b acetate Norethisterone enanthate 17b enanthate Noretynodrel d5 10 NET Norgestrienone d9 11 NET Quingestanol acetate NET 17b acetate 3 cyclopentyl enol ether Tibolone 7a methyl d5 10 NET Gonanes Desogestrel 3 deketo 11 methylene 18 methyl NET Etonogestrel 11 methylene 18 methyl NET Gestodene 18 methyl d15 NET Gestrinone 18 methyl d9 11 NET Levonorgestrel 18 methyl NET Norelgestromin 18 methyl NET 3 oxime Norgestimate 18 methyl NET 3 oxime 17b acetate Norgestrel 13 ethyl NET Several of these act as prodrugs of norethisterone including NETA NETE etynodiol diacetate lynestrenol and quingestanol acetate 105 106 107 Noretynodrel may also be a prodrug of norethisterone 3 1 NETA is taken by mouth similarly to norethisterone while NETE is given by injection into muscle 10 Non 17a ethynylated edit 19 Nortestosterone 19 NT progestins which are technically not derivatives of norethisterone as they do not have a C17a ethynyl group but are still closely related with other substitutions at the C17a and or C16b positions include the following marketed medications 101 27 The C17a vinyl ethenyl derivatives norgesterone 17a vinyl d5 10 19 NT and norvinisterone 17a vinyl 19 NT The C17a allyl derivatives allylestrenol 3 deketo 17a allyl 19 NT and altrenogest 17a allyl d9 11 19 NT The C17a alkyl derivative normethandrone 17a methyl 19 NT The C17a cyanomethyl derivative dienogest 17a cyanomethyl d9 19 NT The C16b ethyl derivative oxendolone 16b ethyl 19 NT Many anabolic steroids of the 19 nortestosterone family like norethandrolone and ethylestrenol are also potent progestogens but were never marketed as such Synthesis edit Chemical syntheses of norethisterone have been published 101 84 Synthesis 1 edit nbsp Norethisterone synthesis 1 11 108 Estradiol 3 methyl ether 1 EME is partially reduced to the 1 5 diene 2 as also occurs for the first step in the synthesis of nandrolone Oppenauer oxidation then transforms the C17b hydroxyl group into a ketone functionality 3 This is then reacted with metal acetylide into the corresponding C17a ethynyl compound 4 Hydrolysis of the enol ether under mild conditions leads directly to 5 108 which appears to be noretynodrel although Lednicer states that it is etynodrel in his book which may be a synonym etynodiol etynodrel is with a chlorine atom attached an orally active progestin This is the progestogen component of the first oral contraceptive to be offered for sale i e Enovid Treatment of the ethynyl enol ether with strong acid leads to norethisterone 6 11 In practice these and all other combined oral contraceptives are mixtures of 1 to 2 EE or mestranol and an oral progestin It has been speculated that the discovery of the necessity of estrogen in addition to progestin for contraceptive efficacy is due to the presence of a small amount of unreduced EME 1 in early batches of 2 This when subjected to oxidation and ethynylation would of course lead to mestranol 3 In any event the need for the presence of estrogen in the mixture is now well established experimentally Synthesis 2 edit nbsp Norethisterone synthesis 2 109 110 111 112 113 Norethisterone is made from estr 4 ene 3 17 dione bolandione which in turn is synthesized by partial reduction of the aromatic region of the 3 O methyl ether of estrone with lithium in liquid ammonia and simultaneously of the keto group at C17a to a hydroxyl group which is then oxidized back to a keto group by chromium trioxide in acetic acid The conjugated C4 C5 olefin and the carbonyl group at C3 is then transformed to dienol ethyl ether using ethyl orthoformate The obtained product is ethynylated by acetylene in the presence of potassium tert butoxide After hydrochloride hydrolysis of the formed O potassium derivative during which the enol ether is also hydrolyzed and the remaining double bond is shifted the desired norethisterone is obtained History editNorethisterone was synthesized for the first time by chemists Luis Miramontes Carl Djerassi and George Rosenkranz at Syntex in Mexico City in 1951 11 It was derived from ethisterone and was found to possess about 20 fold greater potency as a progestogen in comparison citation needed Norethisterone was the first highly active oral progestogen to be synthesized and was preceded as a progestogen by progesterone 1934 ethisterone 1938 19 norprogesterone 1944 and 17a methylprogesterone 1949 as well as by nandrolone 1950 whereas noretynodrel 1952 and norethandrolone 1953 followed the synthesis of norethisterone 12 13 The drug was introduced as Norlutin in the United States in 1957 14 Norethisterone was subsequently combined with mestranol and marketed as Ortho Novum in the United States in 1963 It was the second progestin after noretynodrel in 1960 to be used in an oral contraceptive 13 In 1964 additional contraceptive preparations containing norethisterone in combination with mestranol or EE such as Norlestrin and Norinyl were marketed in the United States 13 Society and culture editGeneric names edit Norethisterone is the INNTooltip International Nonproprietary Name and BANTooltip British Approved Name of the drug while norethindrone is its USANTooltip United States Adopted Name 101 27 Brand names edit Norethisterone is available in Bangladesh as Menogia ACI Normens Renata etc Norethisterone NET including as NETA and NETE has been marketed under many brand names throughout the world 27 19 Availability edit United States edit See also List of progestogens available in the United States Norethisterone was previously available alone in 5 mg tablets under the brand names Norlutin in the United States but this formulation has since been discontinued in this country 26 However NETA remains available alone in 5 mg tablets under the brand name Aygestin in the United States 26 It is one of the only non contraceptive progestogen only drug formulations that remains available in the United States 26 The others include progesterone medroxyprogesterone acetate megestrol acetate and hydroxyprogesterone caproate as well as the atypical agent danazol 26 Both norethisterone and NETA are also available in the United States as contraceptives 26 Norethisterone is available both alone brand names Camila Errin Heather Micronor Nor QD others and in combination with EE Norinyl Ortho Novum others or mestranol Norinyl Ortho Novum others while NETA is available only in combination with EE Norlestrin others 26 NETE is not available in the United States in any form 26 114 115 Research editNorethisterone as NETA and NETE has been studied for use as a potential male hormonal contraceptive in combination with testosterone in men 116 117 Long acting norethisterone microspheres for intramuscular injection have been studied for potential use in birth control 118 References edit a b c d e f g h Stanczyk FZ September 2002 Pharmacokinetics and potency of progestins used for hormone replacement therapy and contraception Reviews in Endocrine amp Metabolic Disorders 3 3 211 24 doi 10 1023 A 1020072325818 PMID 12215716 S2CID 27018468 a b Fotherby K August 1996 Bioavailability of orally administered sex steroids used in oral contraception and hormone replacement therapy Contraception 54 2 59 69 doi 10 1016 0010 7824 96 00136 9 PMID 8842581 a b c d e f g h i j k l m n o p q r s t u v w x y z aa ab ac ad ae af ag ah ai aj ak al am an Kuhl H August 2005 Pharmacology of estrogens and progestogens influence of different routes of administration PDF Climacteric 8 Suppl 1 3 63 doi 10 1080 13697130500148875 PMID 16112947 S2CID 24616324 Archived PDF from the original on 22 August 2016 Retrieved 6 September 2018 a b c d Korhonen T Turpeinen M Tolonen A Laine K Pelkonen O May 2008 Identification of the human cytochrome P450 enzymes involved in the in vitro biotransformation of lynestrenol and norethindrone The Journal of Steroid Biochemistry and Molecular Biology 110 1 2 56 66 doi 10 1016 j jsbmb 2007 09 025 PMID 18356043 S2CID 10809537 a b c d Taitel HF Kafrissen ME 1995 Norethindrone a review of therapeutic applications International Journal of Fertility and Menopausal Studies 40 4 207 23 PMID 8520623 Alden KR Lowdermilk DL Cashion MC Perry SE 27 December 2013 Maternity and Women s Health Care E Book Elsevier Health Sciences pp 135 ISBN 978 0 323 29368 6 Archived from the original on 9 March 2023 Retrieved 8 January 2018 a b Kuhl H September 1990 Pharmacokinetics of oestrogens and progestogens Maturitas 12 3 171 197 doi 10 1016 0378 5122 90 90003 o PMID 2170822 https www accessdata fda gov drugsatfda docs label 2007 018405s023lbl pdf Archived 10 February 2017 at the Wayback Machine bare URL PDF a b c d e f g Jacobson BD October 1962 Hazards of norethindrone therapy during pregnancy American Journal of Obstetrics and Gynecology 84 7 962 8 doi 10 1016 0002 9378 62 90075 3 PMID 14450719 a b c d IARC Working Group on the Evaluation of Carcinogenic Risks to Humans World Health Organization International Agency for Research on Cancer 2007 Combined Estrogen progestogen Contraceptives and Combined Estrogen progestogen Menopausal Therapy World Health Organization pp 417 ISBN 978 92 832 1291 1 Archived from the original on 10 January 2023 Retrieved 12 October 2016 Norethisterone and its acetate and enanthate esters are progestogens that have weak estrogenic and androgenic properties a b c d Djerassi C Miramontes L Rosenkranz G Sondheimer F Longo LD January 2006 Steroids LIV Synthesis of 19 nor 17alpha ethynyltestosterone and 19 nor 17alpha methyltestosterone 1954 American Journal of Obstetrics and Gynecology 194 1 289 discussion 290 doi 10 1021 ja01645a010 PMID 16389045 a b Shoupe D 7 November 2007 The Handbook of Contraception A Guide for Practical Management Springer Science amp Business Media pp 15 ISBN 978 1 59745 150 5 a b c d e Marks L 2010 Sexual Chemistry A History of the Contraceptive Pill Yale University Press pp 74 76 ISBN 978 0 300 16791 7 a b William Andrew Publishing 22 October 2013 Pharmaceutical Manufacturing Encyclopedia 3rd Edition Elsevier pp 2935 ISBN 978 0 8155 1856 3 Hatcher RA Nelson AL 2007 Contraceptive Technology Ardent Media pp 195 ISBN 978 1 59708 001 9 Archived from the original on 10 January 2023 Retrieved 8 January 2018 Gunasheela S 14 March 2011 Practical Management of Gynecological Problems JP Medical Ltd pp 31 ISBN 978 93 5025 240 6 Archived from the original on 9 March 2023 Retrieved 8 January 2018 Grimes DA Lopez LM O Brien PA Raymond EG November 2013 Progestin only pills for contraception The Cochrane Database of Systematic Reviews 11 CD007541 doi 10 1002 14651858 CD007541 pub3 PMID 24226383 Hussain SF February 2004 Progestogen only pills and high blood pressure is there an 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high myotrophic activity exhibit myotrophic androgenic dissociation since due to changes introduced in the structure of ring A they will probably not be substrates for the 5a reductases 85 5a Reduction does not always amplify the androgenic potency in spite of high RBA of androgens to the AR This is the case for norethisterone Fig 1 34 a synthetic 19 nor 17a ethynyl testosterone derivative which also undergoes enzyme mediated 5a reduction and exerts potent androgenic effects in target organs 5a Reduced norethisterone displays a higher AR binding but shows a significantly lower androgenic potency than unchanged norethisterone 102 103 a b c Lemus AE Enriquez J Garcia GA Grillasca I Perez Palacios G January 1997 5alpha reduction of norethisterone enhances its binding affinity for androgen receptors but diminishes its androgenic potency The Journal of Steroid Biochemistry and Molecular Biology 60 1 2 121 9 doi 10 1016 s0960 0760 96 00172 0 PMID 9182866 S2CID 33771349 Filshie M Guillebaud J 22 October 2013 Contraception Science and Practice Elsevier Science pp 26 ISBN 978 1 4831 6366 6 Norethisterone binds to SHBG with less affinity than endogenous androgens and oestrogens Azziz R 8 November 2007 Androgen Excess Disorders in Women Springer Science amp Business Media pp 124 ISBN 978 1 59745 179 6 Kuiper GG Carlsson B Grandien K Enmark E Haggblad J Nilsson S Gustafsson JA March 1997 Comparison of the ligand binding specificity and transcript tissue distribution of estrogen receptors alpha and beta Endocrinology 138 3 863 70 doi 10 1210 endo 138 3 4979 PMID 9048584 Wiegratz I Kuhl H September 2006 Metabolic and clinical effects of progestogens The European Journal of Contraception amp Reproductive Health Care 11 3 153 61 doi 10 1080 13625180600772741 PMID 17056444 S2CID 27088428 a b Giatti S Melcangi RC Pesaresi M August 2016 The other side of progestins effects in the brain Journal of Molecular Endocrinology 57 2 R109 26 doi 10 1530 JME 16 0061 PMID 27339142 a b c Yamamoto T Tamura T Kitawaki J Osawa Y Okada H June 1994 Suicide inactivation of aromatase in human placenta and uterine leiomyoma by 5 alpha dihydronorethindrone a metabolite of norethindrone and its effect on steroid producing enzymes European Journal of Endocrinology 130 6 634 40 doi 10 1530 eje 0 1300634 PMID 8205267 Perusquia M Villalon CM Navarrete E Garcia GA Perez Palacios G Lemus AE August 2003 Vasodilating effect of norethisterone and its 5 alpha metabolites a novel nongenomic action European Journal of Pharmacology 475 1 3 161 9 doi 10 1016 s0014 2999 03 02106 x PMID 12954372 a b Neubauer H Ma Q Zhou J Yu Q Ruan X Seeger H et al October 2013 Possible role of PGRMC1 in breast cancer development Climacteric 16 5 509 13 doi 10 3109 13697137 2013 800038 PMID 23758160 S2CID 29808177 Trabert B Sherman ME Kannan N Stanczyk FZ April 2020 Progesterone and Breast Cancer Endocrine Reviews 41 2 320 344 doi 10 1210 endrev bnz001 PMC 7156851 PMID 31512725 Anderson RA Baird DT December 2002 Male contraception PDF Endocrine Reviews 23 6 735 62 doi 10 1210 er 2002 0002 PMID 12466187 Archived PDF from the original on 28 August 2021 Retrieved 11 December 2019 a b Kamischke A Nieschlag E January 2004 Progress towards hormonal male contraception Trends in Pharmacological Sciences 25 1 49 57 doi 10 1016 j tips 2003 11 009 PMID 14723979 Rudel HW September 1968 Pharmacology of oral contraceptives Clinical Obstetrics and Gynecology 11 3 632 44 doi 10 1097 00003081 196811030 00002 PMID 4878826 Stanczyk FZ November 2003 All progestins are not created equal Steroids 68 10 13 879 90 doi 10 1016 j steroids 2003 08 003 PMID 14667980 S2CID 44601264 Endrikat J Gerlinger C Richard S Rosenbaum P Dusterberg B December 2011 Ovulation inhibition doses of progestins a systematic review of the available literature and of marketed preparations worldwide Contraception 84 6 549 57 doi 10 1016 j contraception 2011 04 009 PMID 22078182 Shoupe D 1993 Injectable Contraceptives and Contraceptive Vaginal Rings Contraception Clinical Perspectives in Obstetrics and Gynecology Springer pp 144 157 doi 10 1007 978 1 4612 2730 4 13 ISBN 978 1 4612 7645 6 ISSN 0178 0328 Weiner E Johansson ED April 1975 Plasma levels of norethindrone after i m injection of 200 mg norethindrone enanthate Contraception 11 4 419 25 doi 10 1016 0010 7824 75 90004 9 PMID 1122756 Fotherby K Howard G Shrimanker K Elder M Bye PG December 1977 Effect of norethisterone oenanthate on serum gonadotrophin levels Contraception 16 6 591 604 doi 10 1016 0010 7824 77 90060 9 PMID 606499 Goebelsmann U Stanczyk FZ Brenner PF Goebelsmann AE Gentzschein EK Mishell DR March 1979 Serum norethindrone NET concentrations following intramuscular NET enanthate injection Effect upon serum LH FSH estradiol and progesterone Contraception 19 3 283 313 doi 10 1016 0010 7824 79 90022 2 PMID 572279 a b Neumann F Diallo FA Hasan SH Schenck B Traore I 1976 The influence of pharmaceutical compounds on male fertility Andrologia 8 3 203 235 doi 10 1111 j 1439 0272 1976 tb02137 x PMID 793446 S2CID 24859886 Heller CG Laidlaw WM Harvey HT Nelson WO July 1958 Effects of progestational compounds on the reproductive processes of the human male Annals of the New York Academy of Sciences 71 5 649 65 doi 10 1111 j 1749 6632 1958 tb54641 x PMID 13583821 S2CID 32637425 Heller CG Moore DJ Paulsen CA Nelson WO Laidlaw WM December 1959 Effects of progesterone and synthetic progestins on the reproductive physiology of normal men Federation Proceedings 18 1057 65 PMID 14400846 Archived from the original on 18 December 2018 Retrieved 11 December 2019 Paulsen CA March 1965 Progestin Metabolism Special Reference to Estrogenic Pathways Metabolism 14 3 SUPPL 313 9 doi 10 1016 0026 0495 65 90018 1 PMID 14261416 Moudgal NR Suresh R 1995 Some thoughts on development of chemically based male contraceptives PDF Current Science Bangalore 68 4 470 474 ISSN 0011 3891 Archived from the original PDF on 11 December 2019 Retrieved 11 December 2019 Johonsson ED Nygren KG 1973 Depression of plasma testosterone levels in men with norethindrone Contraception 8 3 219 226 doi 10 1016 0010 7824 73 90032 2 ISSN 0010 7824 Zitzmann M Rohayem J Raidt J Kliesch S Kumar N Sitruk Ware R Nieschlag E May 2017 Impact of various progestins with or without transdermal testosterone on gonadotropin levels for non invasive hormonal male contraception a randomized clinical trial Andrology 5 3 516 526 doi 10 1111 andr 12328 PMID 28189123 S2CID 41502711 a b c d Alvarez BD 11 May 2011 Efecto de una Dosis de 50 mg de Enantato de Noretisterona y 5 mg de Valerato de Estradiol en los Niveles de Testosterona Total en Hombres Mexicanos Sanos Effect of a Dose of 50 mg of Norethisterone Enanthate and 5 mg of Estradiol Valerate on Total Testosterone Levels in Healthy Mexican Men MSc National Polytechnic Institute of Mexico Archived from the original on 16 September 2022 Retrieved 12 September 2022 Amory JK 2003 Androgens and Male Contraception Androgens in Health and Disease Contemporary Endocrinology Humana Press pp 405 417 doi 10 1007 978 1 59259 388 0 21 ISBN 978 1 61737 314 5 Kamischke A Diebacker J Nieschlag E September 2000 Potential of norethisterone enanthate for male contraception pharmacokinetics and suppression of pituitary and gonadal function Clinical Endocrinology 53 3 351 358 doi 10 1046 j 1365 2265 2000 01097 x PMID 10971453 S2CID 70515136 Petry R Mauss J Senge T Rausch Stroomann JG 1970 Influence of Cyproterone acetate Norethisterone enanthate and Gestonorone capronate on the Hypophyseal Gonadal Axis in the Male Uber den Einfluss von Cyproteronacetat Norethisterononanthat und Gestonoroncapronat auf die Hypophysen Gonadenachse beim Mann Influence of Cyproterone acetate Norethisterone enanthate and Gestonorone capronate on the Hypophyseal Gonadal Axis in the Male Symposion der Deutschen Gesellschaft fur Endokrinologie in Ulm vom 26 28 Februar 1970 Springer pp 428 430 doi 10 1007 978 3 642 80591 2 118 ISBN 9783642805912 a href Template Cite book html title Template Cite book cite book a journal ignored help a b Die Gestagene Springer Verlag 27 November 2013 pp 13 14 283 284 ISBN 978 3 642 99941 3 Archived from the original on 10 January 2023 Retrieved 19 September 2018 Saperstein S Edgren RA Jung D Mroszczak EJ Lee GJ Dorr A Pritchard R Kushinsky S Fong JC Combs DL December 1989 Pharmacokinetics of norethindrone effect of particle size Contraception 40 6 731 40 doi 10 1016 0010 7824 89 90075 9 PMID 2620531 Friedrich C Berse M Klein S Rohde B Hochel J June 2018 In Vivo Formation of Ethinylestradiol After Intramuscular Administration of Norethisterone Enantate Journal of Clinical Pharmacology 58 6 781 789 doi 10 1002 jcph 1079 PMID 29522253 S2CID 3813229 Thijssen JH September 1972 Metabolism of Orally Active Synthetic Progestational Compounds In Tausk M ed Pharmacology of the Endocrine System and Related Drugs Progesterone Progestational Drugs and Antifertility Agents Vol II Pergamon Press pp 217 273 ISBN 978 0080168128 OCLC 278011135 Okada H 2010 Receptors and Mechanism Action of Synthetic Progestogens Asia Oceania Journal of Obstetrics and Gynaecology 7 1 15 27 doi 10 1111 j 1447 0756 1981 tb00511 x ISSN 0389 2328 Briggs MH 1980 Comparative Pharmacodynamics and Pharmacokinetics of Contraceptive Steroids in Animals and Man A Selective Review Clinical Pharmacology amp Therapeutics Palgrave Macmillan UK pp 493 518 doi 10 1007 978 1 349 05952 2 57 ISBN 978 1 349 05954 6 Thomas JA Keenan EJ 1986 Progestins and Oral Contraceptives Principles of Endocrine Pharmacology Springer pp 167 196 doi 10 1007 978 1 4684 5036 1 8 ISBN 978 1 4684 5036 1 Orme ML Back DJ Breckenridge AM 1983 Clinical pharmacokinetics of oral contraceptive steroids Clinical Pharmacokinetics 8 2 95 136 doi 10 2165 00003088 198308020 00001 PMID 6342899 S2CID 43298472 Fotherby K 1974 Metabolism of synthetic steroids by animals and man Acta Endocrinologica Supplementum 185 119 147 doi 10 1530 acta 0 075s119 PMID 4206183 Kuhl H Wiegratz I August 2007 Can 19 nortestosterone derivatives be aromatized in the liver of adult humans Are there clinical implications Climacteric 10 4 344 353 doi 10 1080 13697130701380434 PMID 17653961 S2CID 20759583 Stanczyk FZ Roy S July 1990 Metabolism of levonorgestrel norethindrone and structurally related contraceptive steroids Contraception 42 1 67 96 doi 10 1016 0010 7824 90 90093 B PMID 2143719 a b Schoonen WG Deckers GH de Gooijer ME de Ries R Kloosterboer HJ November 2000 Hormonal properties of norethisterone 7alpha methyl norethisterone and their derivatives The Journal of Steroid Biochemistry and Molecular Biology 74 4 213 22 doi 10 1016 s0960 0760 00 00125 4 PMID 11162927 S2CID 19797254 several mono and disulphated as well as mono and diglucuronidated metabolites of NET have been detected in urine from NET treated women 16 17 In unconjugated form these NET or MeNET metabolites are represented by 5a and 5b reduced NET 5a NET or 5b NET and by 3a and 3b hydrogenated 5a NET and 5b NET leading to 3a 5a NET 3b 5a NET 3a 5b NET and 3b 5b NET or their corresponding MeNET metabolites Figs 1 and 2 These steroid conversions of NET or MeNET may take place in the liver but also in the pituitary endometrium prostate vagina and breast The enzymes involved in these metabolic processes are 5a and 5b reductase as well as 3a and 3b hydroxysteroid dehydrogenase HSD Chavez BA Vilchis F Perez AE Garcia GA Grillasca I Perez Palacios G January 1985 Stereospecificity of the intracellular binding of norethisterone and its A ring reduced metabolites Journal of Steroid Biochemistry 22 1 121 6 doi 10 1016 0022 4731 85 90151 7 PMID 3871879 Garza Flores J Vilchis F Garcia GA Menjivar M Perez Palacios G June 1986 A ring reduction enhances the antigonadotropic potency of norethisterone Acta Endocrinologica 112 2 278 83 doi 10 1530 acta 0 1120278 PMID 3090814 Lemus AE Enriquez J Hernandez A Santillan R Perez Palacios G February 2009 Bioconversion of norethisterone a progesterone receptor agonist into estrogen receptor agonists in osteoblastic cells The Journal of Endocrinology 200 2 199 206 doi 10 1677 JOE 08 0166 PMID 19008332 Scarsi KK Darin KM Chappell CA Nitz SM Lamorde M November 2016 Drug Drug Interactions Effectiveness and Safety of Hormonal Contraceptives in Women Living with HIV Drug Safety 39 11 1053 1072 doi 10 1007 s40264 016 0452 7 PMC 5048570 PMID 27562873 DeGroot LJ 2001 Endocrinology W B Saunders Co p 2617 ISBN 978 0 7216 7843 6 a b c d e Elks J 14 November 2014 The Dictionary of Drugs Chemical Data Chemical Data Structures and Bibliographies Springer pp 886 ISBN 978 1 4757 2085 3 Archived from the original on 10 January 2023 Retrieved 5 October 2016 Chwalisz K Surrey E Stanczyk FZ June 2012 The hormonal profile of norethindrone acetate rationale for add back therapy with gonadotropin releasing hormone agonists in women with endometriosis Reproductive Sciences 19 6 563 71 doi 10 1177 1933719112438061 PMID 22457429 S2CID 2882899 Shoupe D Haseltine FP 6 December 2012 Contraception Springer Science amp Business Media pp 112 ISBN 978 1 4612 2730 4 Ryan KJ 1999 Kistner s Gynecology and Women s Health Mosby p 292 ISBN 978 0 323 00201 1 Hammerstein J December 1990 Prodrugs advantage or disadvantage American Journal of Obstetrics and Gynecology 163 6 Pt 2 2198 203 doi 10 1016 0002 9378 90 90561 K PMID 2256526 Edelman AB Cherala G Stanczyk FZ October 2010 Metabolism and pharmacokinetics of contraceptive steroids in obese women a review Contraception 82 4 314 23 doi 10 1016 j contraception 2010 04 016 PMID 20851224 Raynaud JP Ojasoo T November 1986 The design and use of sex steroid antagonists Journal of Steroid Biochemistry 25 5B 811 33 doi 10 1016 0022 4731 86 90313 4 PMID 3543501 Similar androgenic potential is inherent to norethisterone and its prodrugs norethisterone acetate ethynodiol diacetate lynestrenol norethynodrel quingestanol acetate a b Frank B Colton U S patent 2 655 518 1952 to Searle amp Co Ringold HJ Rosenkranz G Sondheimer F 1956 Steroids LXXX 11 Methyl 19 nortestosterone and 1 Methyl 17a ethinyl 19 nortestosterone Journal of the American Chemical Society 78 11 2477 2479 doi 10 1021 ja01592a037 Ueberwasser H Heusler K Kalvoda J Meystre C Wieland P Anner G Wettstein A 1963 19 Norsteroide II Ein einfaches Herstellungsverfahren fur 19 Norandrostan Derivate uber Steroide 193 Mitteilung Helvetica Chimica Acta 46 344 352 doi 10 1002 hlca 19630460135 Onken D Heublein D January 1970 Ethinylated steroids Die Pharmazie 25 1 3 9 PMID 4914401 U S patent 2 744 122 U S patent 2 774 777 Bullough VL 2001 Encyclopedia of Birth Control ABC CLIO pp 145 ISBN 978 1 57607 181 6 Archived from the original on 10 January 2023 Retrieved 27 November 2016 Moskowitz EH Jennings B 13 September 1996 Coerced Contraception Moral and Policy Challenges of Long Acting Birth Control Georgetown University Press pp 40 ISBN 978 1 58901 807 5 Nieschlag E November 2010 Clinical trials in male hormonal contraception PDF Contraception 82 5 457 70 doi 10 1016 j contraception 2010 03 020 PMID 20933120 Archived PDF from the original on 5 December 2020 Retrieved 28 December 2018 Nieschlag E Behre HM Nieschlag E Behre HM Nieschlag S 2012 Nieschlag E Behre HM Nieschlag S eds The essential role of testosterone in hormonal male contraception Testosterone 470 493 doi 10 1017 CBO9781139003353 023 ISBN 9781139003353 Benagiano G Primiero FM June 1983 Long acting contraceptives Present status Drugs 25 6 570 609 doi 10 2165 00003495 198325060 00003 PMID 6223801 S2CID 45898359 Further reading editBrogden RN Speight TM Avery GS 1973 Progestagen only oral contraceptives a preliminary report of the action and clinical use of norgestrel and norethisterone Drugs 6 3 169 81 doi 10 2165 00003495 197306030 00004 PMID 4130566 S2CID 42295736 Norethisterone and norethisterone acetate IARC Monographs on the Evaluation of the Carcinogenic Risk of Chemicals to Humans 21 441 60 December 1979 PMID 120838 Stanczyk FZ Roy S July 1990 Metabolism of levonorgestrel norethindrone and structurally related contraceptive steroids Contraception 42 1 67 96 doi 10 1016 0010 7824 90 90093 b PMID 2143719 Wiseman LR McTavish D March 1994 Transdermal estradiol norethisterone A review of its pharmacological properties and clinical use in postmenopausal women Drugs amp Aging 4 3 238 56 doi 10 2165 00002512 199404030 00006 PMID 8199397 S2CID 68007924 Taitel HF Kafrissen ME 1995 Norethindrone a review of therapeutic applications International Journal of Fertility and Menopausal Studies 40 4 207 23 PMID 8520623 Maier WE Herman JR August 2001 Pharmacology and toxicology of ethinyl estradiol and norethindrone acetate in experimental animals Regulatory Toxicology and Pharmacology 34 1 53 61 doi 10 1006 rtph 2001 1483 PMID 11502156 Riis BJ Lehmann HJ Christiansen C October 2002 Norethisterone acetate in combination with estrogen effects on the skeleton and other organs A review American Journal of Obstetrics and Gynecology 187 4 1101 16 doi 10 1067 mob 2002 122852 PMID 12389012 Draper BH Morroni C Hoffman M Smit J Beksinska M Hapgood J Van der Merwe L July 2006 Depot medroxyprogesterone versus norethisterone oenanthate for long acting progestogenic contraception The Cochrane Database of Systematic Reviews 3 CD005214 doi 10 1002 14651858 CD005214 pub2 PMID 16856087 Kuhl H Wiegratz I August 2007 Can 19 nortestosterone derivatives be aromatized in the liver of adult humans Are there clinical implications Climacteric 10 4 344 53 doi 10 1080 13697130701380434 PMID 17653961 S2CID 20759583 Casey CL Murray CA 2008 HT update spotlight on estradiol norethindrone acetate combination therapy Clinical Interventions in Aging 3 1 9 16 doi 10 2147 cia s1663 PMC 2544373 PMID 18488874 Paulen ME Curtis KM October 2009 When can a woman have repeat progestogen only injectables depot medroxyprogesterone acetate or norethisterone enantate Contraception 80 4 391 408 doi 10 1016 j contraception 2009 03 023 PMID 19751863 Chwalisz K Surrey E Stanczyk FZ June 2012 The hormonal profile of norethindrone acetate rationale for add back therapy with gonadotropin releasing hormone agonists in women with endometriosis Reproductive Sciences 19 6 563 71 doi 10 1177 1933719112438061 PMID 22457429 S2CID 2882899 Portal nbsp Medicine Retrieved from https en wikipedia org w index php title Norethisterone amp oldid 1205246352, wikipedia, wiki, book, books, library,

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