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Progesterone

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Progesterone

Systematic (IUPAC) name

Pregn-4-ene-3,20-dione

Clinical data Trade names AHFS/Drugs.com MedlinePlus Pregnancy cat. Legal status Crinone, Endometrin monograph a604017 B (USA) ?

Routes

oral, implant Pharmacokinetic data

Bioavailability

prolonged absorption, half-life approx 25-50 hours

Protein binding Metabolism

96%-99% hepatic to pregnanediols and pregnanolones

Half-life Excretion

34.8-55.13 hours renal Identifiers

CAS number ATC code PubChem IUPHAR ligand DrugBank ChemSpider UNII KEGG ChEBI

57-83-0 G03DA04 CID 5994 2377 DB00396 5773 4G7DS2Q64Y D00066 CHEBI:17026

ChEMBL Synonyms

CHEMBL103 4-pregnene-3,20-dione Chemical data

Formula Mol. mass SMILES InChI

C201H300O200 314.46 eMolecules & PubChem

InChI=1S/C21H30O2/c1-13(22)17-6-7-18-16-5-4-14-1215(23)8-10-20(14,2)19(16)9-11-21(17,18)3/h12,16-19H,411H2,1-3H3/t16-,17+,18-,19-,20-,21+/m0/s1 Key:RJKFOVLPORLFTN-LEKSSAKUSA-N Physical data Melt. point Spec. rot 126 C (259 F) []D (what is this?) (verify)

Progesterone also known as P4 (pregn-4-ene-3,20-dione) is a C-21 steroid hormone involved in the female menstrual cycle, pregnancy (supports gestation) and embryogenesis of humans and other species. Progesterone belongs to a class of hormones called progestogens, and is the major naturally occurring human progestogen. Progesterone is commonly manufactured from the yam family, Dioscorea. Dioscorea produces large amounts of a steroid called diosgenin, which can be converted into progesterone in the laboratory.

Contents

1 Chemistry 2 Sources o 2.1 Animal o 2.2 Plants

3 Synthesis o 3.1 Biosynthesis o 3.2 Laboratory 4 Levels 5 Effects o 5.1 Reproductive system o 5.2 Nervous system o 5.3 Other syndromes 6 Adverse effects 7 Medical applications o 7.1 Bioavailability o 7.2 Specific uses o 7.3 Aging o 7.4 Brain damage 8 See also 9 References 10 Additional images 11 External links

[edit] Chemistry
Progesterone was independently discovered by four research groups.[1][2][3][4] Willard Myron Allen co-discovered progesterone with his anatomy professor George Washington Corner at the University of Rochester Medical School in 1933. Allen first determined its melting point, molecular weight, and partial molecular structure. He also gave it the name Progesterone derived from Progestational Steroidal ketone.[5] 0 Like other steroids, progesterone consists of four interconnected cyclic hydrocarbons. Progesterone contains ketone and oxygenated functional groups, as well as two methyl branches. Like all steroid hormones, it is hydrophobic.

[edit] Sources
[edit] Animal
Progesterone is produced in the ovaries (to be specific, after ovulation in the corpus luteum), the adrenal glands (near the kidney), and, during pregnancy, in the placenta. Progesterone is also stored in adipose (fat) tissue. In humans, increasing amounts of progesterone are produced during pregnancy:

At first, the source is the corpus luteum that has been "rescued" by the presence of human chorionic gonadotropins (hCG) from the conceptus.

However, after the 8th week, production of progesterone shifts to the placenta. The placenta utilizes maternal cholesterol as the initial substrate, and most of the produced progesterone enters the maternal circulation, but some is picked up by the fetal circulation and used as substrate for fetal corticosteroids. At term the placenta produces about 250 mg progesterone per day. An additional source of progesterone is milk products. After consumption of milk products the level of bioavailable progesterone goes up.[6]

[edit] Plants
In at least one plant, Juglans regia, progesterone has been detected.[7] In addition, progesterone-like steroids are found in Dioscorea mexicana. Dioscorea mexicana is a plant that is part of the yam family native to Mexico.[8] It contains a steroid called diosgenin that is taken from the plant and is converted into progesterone.[9] Diosgenin and progesterone are found in other Dioscorea species as well. Another plant that contains substances readily convertible to progesterone is Dioscorea pseudojaponica native to Taiwan. Research has shown that the Taiwanese yam contains saponins steroids that can be converted to diosgenin and thence to progesterone.[10] Many other Dioscorea species of the yam family contain steroidal substances from which progesterone can be produced. Among the more notable of these are Dioscorea villosa and Dioscorea polygonoides. One study showed that the Dioscorea villosa contains 3.5% diosgenin.[11] Dioscorea polygonoides has been found to contain 2.64% diosgenin as shown by gas chromatography-mass spectrometry.[12] Many of the Dioscorea species that originate from the yam family grow in countries that have tropical and subtropical climates.[13]

[edit] Synthesis
[edit] Biosynthesis

Top: Conversion of cholesterol (1) into pregnenolone (3) to progesterone (6). Bottom: Progesterone is important for aldosterone (mineralocorticoid) synthesis, as 17hydroxyprogesterone is for cortisol (glucocorticoid), and androstenedione for sex steroids. In mammals, progesterone (6), like all other steroid hormones, is synthesized from pregnenolone (3), which in turn is derived from cholesterol (1) (see the upper half of the figure to the right). Cholesterol (1) undergoes double oxidation to produce 20,22-dihydroxycholesterol (2). This vicinal diol is then further oxidized with loss of the side chain starting at position C22 to produce pregnenolone (3). This reaction is catalyzed by cytochrome P450scc. The conversion of pregnenolone to progesterone takes place in two steps. First, the 3hydroxyl group is oxidized to a keto group (4) and second, the double bond is moved to C-4, from C-5 through a keto/enol tautomerization reaction.[14] This reaction is catalyzed by 3beta-hydroxysteroid dehydrogenase/delta(5)-delta(4)isomerase. Progesterone in turn (see lower half of figure to the right) is the precursor of the mineralocorticoid aldosterone, and after conversion to 17-hydroxyprogesterone (another natural progestogen) of cortisol and androstenedione. Androstenedione can be converted to testosterone, estrone and estradiol. Pregenolone and progesterone can also be synthesized by yeast.[15]

[edit] Laboratory

The Marker semisynthesis of progesterone from diosgenin.[16] An economical semisynthesis of progesterone from the plant steroid diosgenin isolated from yams was developed by Russell Marker in 1940 for the Parke-Davis pharmaceutical company (see figure to the right).[16] This synthesis is known as the Marker degradation. Additional semisyntheses of progesterone have also been reported starting from a variety of steroids. For the example, cortisone can be simultaneously deoxygenated at the C-17 and C-21 position by treatment with iodotrimethylsilane in chloroform to produce 11keto-progesterone (ketogestin), which in turn can be reduced at position-11 to yield progesterone.[17]

The Johnson total synthesis of progesterone.[18] A total synthesis of progesterone was reported in 1971 by W.S. Johnson (see figure to the right).[18] The synthesis begins with reacting the phosphonium salt 7 with phenyl lithium to produce the phosphonium ylide 8. The ylide 8 is reacted with an aldehyde to produce the alkene 9. The ketal protecting groups of 9 are hydrolyzed to produce the diketone 10, which in turn is cyclized to form the cyclopentenone 11. The ketone of 11 is reacted with methyl lithium to yield the tertiary alcohol 12, which in turn is treated with acid to produce the tertiary cation 13. The key step of the synthesis is the -cation cyclization of 13 in which the B-, C-, and D-rings of the steroid are simultaneously formed to produce 14. This step resembles the cationic cyclization reaction used in the biosynthesis of steroids and hence is referred to as biomimetic. In the next step the enol orthoester is hydrolyzed to produce the ketone 15. The cyclopentene A-ring is then opened by oxidizing with ozone to produce 16. Finally, the diketone 17 undergoes an intramolecular aldol condensation by treating with aqueous potassium hydroxide to produce progesterone.[18]

[edit] Levels
In women, progesterone levels are relatively low during the preovulatory phase of the menstrual cycle, rise after ovulation, and are elevated during the luteal phase, as shown in diagram below. Progesterone levels tend to be < 2 ng/ml prior to ovulation, and > 5 ng/ml after ovulation. If pregnancy occurs, human chorionic gonadotropin is released maintaining the corpus leuteum allowing it to maintain levels of progesterone. At around 12 weeks the placenta begins to produce progesterone in place of the corpus leuteum, this process is named the luteal-placental shift. After the luteal-placental shift progesterone levels start to rise further and may reach 100-200 ng/ml at term. Whether a decrease in progesterone levels is critical for the initiation of labor has been argued and may be species-specific. After delivery of the placenta and during lactation, progesterone levels are very low. Progesterone levels are relatively low in children and postmenopausal women.[19] Adult males have levels similar to those in women during the follicular phase of the menstrual cycle. Reference range for blood test Lower limit Upper limit Unit Female - menstrual cycle (see diagram below) <0.2[20] 1[20] ng/mL Female - postmenopausal [21] [21] <0,6 3 nmol/L [20] [20] 0.34 0.92 ng/mL Female on oral contraceptives [21] [21] 1.1 2.9 nmol/L [20] [20] 0.27 0.9 ng/mL Males 16 years [21] [21] 0.86 2.9 nmol/L [20] [20] [20] 0.1 4.1 or 4.5 ng/mL Female or male 1-9 years [21] 0.3 13[21] nmol/L Person type

Progesterone levels during the menstrual cycle.[22] - The ranges denoted By biological stage may be used in closely monitored menstrual cycles in regard to other markers of its biological progression, with the time scale being

compressed or stretched to how much faster or slower, respectively, the cycle progresses compared to an average cycle. - The ranges denoted Inter-cycle variability are more appropriate to use in nonmonitored cycles with only the beginning of menstruation known, but where the woman accurately knows her average cycle lengths and time of ovulation, and that they are somewhat averagely regular, with the time scale being compressed or stretched to how much a woman's average cycle length is shorter or longer, respectively, than the average of the population. - The ranges denoted Inter-woman variability are more appropriate to use when the average cycle lengths and time of ovulation are unknown, but only the beginning of menstruation is given.

[edit] Effects

Micrograph showing changes to the endometrium due to progesterone (decidualization) H&E stain. Progesterone exerts its primary action through the intracellular progesterone receptor although a distinct, membrane bound progesterone receptor has also been postulated.[23][24] In addition, progesterone is a highly potent antagonist of the mineralocorticoid receptor (MR, the receptor for aldosterone and other mineralocorticosteroids). It prevents MR activation by binding to this receptor with an affinity exceeding even those of aldosterone and other corticosteroids such as cortisol and corticosterone.[25] Progesterone has a number of physiological effects that are amplified in the presence of estrogen. Estrogen through estrogen receptors upregulates the expression of progesterone receptors.[26] Also, elevated levels of progesterone potently reduce the sodium-retaining activity of aldosterone, resulting in natriuresis and a reduction in extracellular fluid volume. Progesterone withdrawal, on the other hand, is associated with a temporary increase in sodium retention (reduced natriuresis, with an increase in extracellular fluid volume) due to the compensatory increase in aldosterone production, which combats the blockade of the mineralocorticoid receptor by the previously elevated level of progesterone.[27]

[edit] Reproductive system

Progesterone has key effects via non-genomic signalling on human sperm as they migrate through the female tract before fertilization occurs, though the receptor(s) as yet remain unidentified.[28] Detailed characterisation of the events occurring in sperm in response to progesterone has elucidated certain events including intracellular calcium transients and maintained changes,[29] slow calcium oscillations,[30] now thought to possibly regulate motility.[31] Interestingly progesterone has also been shown to demonstrate effects on octopus spermatozoa.[32] Progesterone modulates the activity of CatSper (cation channels of sperm) voltage-gated Ca2+ channels. Since eggs release progesterone, sperm may use progesterone as a homing signal to swim toward eggs (chemotaxis). Hence substances that block the progesterone binding site on CatSper channels could potentially be used in male contraception.[33][34] Progesterone is sometimes called the "hormone of pregnancy",[35] and it has many roles relating to the development of the fetus:

Progesterone converts the endometrium to its secretory stage to prepare the uterus for implantation. At the same time progesterone affects the vaginal epithelium and cervical mucus, making it thick and impenetrable to sperm. If pregnancy does not occur, progesterone levels will decrease, leading, in the human, to menstruation. Normal menstrual bleeding is progesterone-withdrawal bleeding. If ovulation does not occur and the corpus luteum does not develop, levels of progesterone may be low, leading to anovulatory dysfunctional uterine bleeding. During implantation and gestation, progesterone appears to decrease the maternal immune response to allow for the acceptance of the pregnancy. Progesterone decreases contractility of the uterine smooth muscle.[35] In addition progesterone inhibits lactation during pregnancy. The fall in progesterone levels following delivery is one of the triggers for milk production. A drop in progesterone levels is possibly one step that facilitates the onset of labor.

The fetus metabolizes placental progesterone in the production of adrenal steroids.

[edit] Nervous system


Progesterone, like pregnenolone and dehydroepiandrosterone, belongs to the group of neurosteroids. It can be synthesized within the central nervous system and also serves as a precursor to another major neurosteroid, allopregnanolone. Neurosteroids affect synaptic functioning, are neuroprotective, and affect myelination.[36] They are investigated for their potential to improve memory and cognitive ability. Progesterone affects regulation of apoptotic genes. Its effect as a neurosteroid works predominantly through the GSK-3 beta pathway, as an inhibitor. (Other GSK-3 beta inhibitors include bipolar mood stabilizers, lithium and valproic acid.)

[edit] Other syndromes


It raises epidermal growth factor-1 levels, a factor often used to induce proliferation, and used to sustain cultures, of stem cells. It increases core temperature (thermogenic function) during ovulation.[37] It reduces spasm and relaxes smooth muscle. Bronchi are widened and mucus regulated. (Progesterone receptors are widely present in submucosal tissue.) It acts as an antiinflammatory agent and regulates the immune response. It reduces gall-bladder activity.[38] It normalizes blood clotting and vascular tone, zinc and copper levels, cell oxygen levels, and use of fat stores for energy. It may affect gum health, increasing risk of gingivitis (gum inflammation) and tooth decay. It appears to prevent endometrial cancer (involving the uterine lining) by regulating the effects of estrogen.

[edit] Adverse effects


Pill form of progesterone (actually a synthetic version such as Progestogen) taken at 400 mg as cited by the following patent can cause increased fluid retention, which may result in epilepsy, migraine, asthma, cardiac or renal dysfunction. Blood clots that can result in strokes and heart attacks, which may lead to death or long-term disability, may develop; pulmonary embolus or breast cancer can also develop as a result of progesterone therapy. Progesterone is associated with an increased risk of thrombotic disorders such as thrombophlebitis, cerebrovascular disorders, pulmonary embolism, and retinal thrombosis.[39] Common adverse effects include cramps, abdominal pain, skeletal pain, perineal pain, headache, arthralgia, constipation, dyspareunia, nocturia, diarrhea, nausea, vomiting, breast enlargement, joint pain, flatulence, hot flushes, decreased libido, thirst, increased appetite, nervousness, drowsiness, excessive urination at night. Psychiatric effects including depression, mood swings, emotional instability, aggression, abnormal crying, insomnia, forgetfulness, sleep disorders.[39] Less frequent adverse effects that may occur include allergy, anemia, bloating, fatigue, tremor, urticaria, pain, conjunctivitis, dizziness, vomiting, myalgia, back pain, breast pain, genital itching, genital yeast infection, upper respiratory tract infection, cystitis, dysuria, asthenia, xerophthalmia, syncope, dysmenorrhea, premenstrual tension, gastritis, urinary tract infection, vaginal discharge, pharyngitis, sweating, hyperventilation, vaginal dryness, dyspnea, fever, edema, flu-like symptoms, dry mouth, rhinitis, leg pain, skin discoloration, skin disorders, seborrhea, sinusitis, acne.[39] Current research suggests that progesterone plays an important role in the signaling of insulin release and pancreatic function, and may affect the susceptibility to diabetes.[40] It has been shown that women with high levels of progesterone during pregnancy are more likely to develop glucose abnormalities.[41]

[edit] Medical applications

Prometrium 100 mg Oral Capsule The use of progesterone and its analogues have many medical applications, both to address acute situations and to address the long-term decline of natural progesterone levels. Because of the poor bioavailability of progesterone when taken orally, many synthetic progestins have been designed with improved oral bioavailability.[42] Progesteone was approved by the United States Food and Drug Administration as vaginal gel on July 31, 1997,[43] an oral capsule on May 14, 1998[44] in an injection form on April 25, 2001[45] and as a vaginal insert on June 21, 2007.[46] In Italy and Spain, Progesterone is sold under the trademark Progeffik.

[edit] Bioavailability
The route of administration impacts the effect of the drug. Given orally, progesterone has a wide person-to-person variability in absorption and bioavailability while synthetic progestins are rapidly absorbed with a longer half-life than progesterone and maintain stable levels in the blood.[47] Progesterone does not dissolve in water and is poorly absorbed when taken orally unless micronized in oil. Products are often sold as capsules containing micronised progesterone in oil. Progesterone can also be administered through vaginal or rectal suppositories or pessaries, transdermally through a gel or cream,[48] or via injection (though the latter has a short half-life requiring daily administration). "Natural progesterone" products derived from yams do not require a prescription, but there is no evidence that the human body can convert its active ingredient (diosgenin, the plant steroid that is chemically converted to produce progesterone industrially[16]) into progesterone.[49][50]

[edit] Specific uses

Progesterone is used to support pregnancy in Assisted Reproductive Technology (ART) cycles such as In-vitro Fertilization (IVF). While daily intramuscular injections of progesterone-in-oil (PIO) have been the standard route of

administration, PIO injections are not FDA-approved for use in pregnancy. A recent meta-analysis showed that the intravaginal route with an appropriate dose and dosing frequency is equivalent to daily intramuscular injections.[51] In addition, a recent case-matched study comparing vaginal progesterone with PIO injections showed that live birth rates were nearly identical with both methods.[52] Progesterone is used to control persistent anovulatory bleeding. It is also used to prepare uterine lining in infertility therapy and to support early pregnancy. Patients with recurrent pregnancy loss due to inadequate progesterone production may receive progesterone. Progesterone is also used in nonpregnant women with a delayed menstruation of one or more weeks, in order to allow the thickened endometrial lining to slough off. This process is termed a progesterone withdrawal bleed. The progesterone is taken orally for a short time (usually one week), after which the progesterone is discontinued and bleeding should occur. Progesterone is being investigated as potentially beneficial in treating multiple sclerosis, since the characteristic deterioration of nerve myelin insulation halts during pregnancy, when progesterone levels are raised; deterioration commences again when the levels drop. Vaginally dosed progesterone is being investigated as potentially beneficial in preventing preterm birth in women at risk for preterm birth. The initial study by Fonseca suggested that vaginal progesterone could prevent preterm birth in women with a history of preterm birth.[53] According to a recent study, women with a short cervix that received hormonal treatment with a progesterone gel had their risk of prematurely giving birth reduced. The hormone treatment was administered vaginally every day during the second half of a pregnancy. [54]

A subsequent and larger study showed that vaginal progesterone was no better than placebo in preventing recurrent preterm birth in women with a history of a previous preterm birth,[55] but a planned secondary analysis of the data in this trial showed that women with a short cervix at baseline in the trial had benefit in two ways: a reduction in births less than 32 weeks and a reduction in both the frequency and the time their babies were in intensive care.[56] In another trial, vaginal progesterone was shown to be better than placebo in reducing preterm birth prior to 34 weeks in women with an extremely short cervix at baseline.[57] An editorial by Roberto Romero discusses the role of sonographic cervical length in identifying patients who may benefit from progesterone treatment.[58]

Progesterone also has a role in skin elasticity and bone strength, in respiration, in nerve tissue and in female sexuality, and the presence of progesterone receptors in certain muscle and fat tissue may hint at a role in sexually-dimorphic proportions of those.[59] Progesterone receptor antagonists, or selective progesterone receptor modulators (SPRM)s, such as RU-486 (Mifepristone), can be used to prevent conception or induce medical abortions.

Note that methods of hormonal contraception do not contain progesterone but a progestin. Progesterone may affect male behavior.[60] Progesterone is starting to be used in the treatment of the skin condition hidradenitis suppurativa.[citation needed]

[edit] Aging
Since most progesterone in males is created during testicular production of testosterone, and most in females by the ovaries, the shutting down (whether by natural or chemical means), or removal, of those inevitably causes a considerable reduction in progesterone levels. Previous concentration upon the role of progestagens (progesterone and molecules with similar effects) in female reproduction, when progesterone was simply considered a "female hormone", obscured the significance of progesterone elsewhere in both sexes. The tendency for progesterone to have a regulatory effect, the presence of progesterone receptors in many types of body tissue, and the pattern of deterioration (or tumor formation) in many of those increasing in later years when progesterone levels have dropped, is prompting widespread research into the potential value of maintaining progesterone levels in both males and females.

[edit] Brain damage


Previous studies have shown that progesterone supports the normal development of neurons in the brain, and that the hormone has a protective effect on damaged brain tissue. It has been observed in animal models that females have reduced susceptibility to traumatic brain injury and this protective effect has been hypothesized to be caused by increased circulating levels of estrogen and progesterone in females.[61] A number of additional animal studies have confirmed that progesterone has neuroprotective effects when administered shortly after traumatic brain injury.[62] Encouraging results have also been reported in human clinical trials.[63][64] The mechanism of progesterone protective effects may be the reduction of inflammation that follows brain trauma.[65]

[edit] See also


Willard Myron Allen Endometrin Prometrium AKR1C1 - the enzyme that deactivates progesterone Percy Julian

[edit] References
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[edit] Additional images

Steroidogenesis, showing progesterone among the progestagens in yellow area.

Pregnenolone

Deoxycorticosterone

[edit] External links


MeSH Progesterone Kimball JW (2007-05-27). "Progesterone". Kimball's Biology Pages. http://users.rcn.com/jkimball.ma.ultranet/BiologyPages/P/Progesterone.html. Retrieved 2008-06-18. "Progesterone Resource Center". PMS, Menopause, and Progesterone Resource Center. Oasis Advanced Wellness, Inc. http://www.pms-menopauseprogesterone.org/progesterone/. Retrieved 2008-06-18. General discussion document on Progesterone, its uses and applications v d eEndocrine system: hormones (Peptide hormones Steroid

hormones)
GnRH TRH Dopamine CRH Hypothalamus GHRH/Somatostatin Melanin concentrating hormone Hypothalamic- Posterior pituitary Vasopressin Oxytocin pituitary (FSH FSHB, LH LHB, TSH TSHB, CGA) Prolactin POMC Anterior pituitary (CLIP, ACTH, MSH, Endorphins, Lipotropin) GH Adrenal axis Endocrine glands Thyroid axis Adrenal cortex: aldosterone cortisol DHEA Adrenal medulla: epinephrine norepinephrine Thyroid: thyroid hormone (T3 and T4) calcitonin Parathyroid: PTH Testis: testosterone AMH inhibin Ovary: estradiol progesterone activin and inhibin relaxin (pregnancy)

Gonadal axis

Placenta: hCG HPL estrogen progesterone Pancreas: glucagon insulin amylin somatostatin Islet-Acinar pancreatic polypeptide Axis Pineal gland: melatonin Thymus: Thymosin (Thymosin 1, Thymosin beta) Thymopoietin Thymulin Non-end. glands Digestive system: Stomach: gastrin ghrelin Duodenum: CCK GIP secretin motilin VIP Ileum: enteroglucagon peptide YY Liver/other: Insulin-like growth factor (IGF-1, IGF-2)

Adipose tissue: leptin adiponectin resistin Skeleton: Osteocalcin Kidney: JGA (renin) peritubular cells (EPO) calcitriol prostaglandin Heart: Natriuretic peptide (ANP, BNP) anat/phys/devp/horm noco(d)/cong/tumr, sysi/epon

M: END

proc, drug (A10/H1/H2/H3/H5)

v d eEstrogens and progestogens (G03C-D, L02) Norpregnene 1st (Norethisterone#/Norethisterone acetate Ethynodiol diacetate) Norpregnene 2nd (Levonorgestrel#/Norgestrel/Norelgestromi n) 19-nortestosterone 3rd (Desogestrel/Etonogestrel Gestodene Norgestimate) Androstene (Drospirenone) 19norprogesterone (Nomegestrol 4th Promegestone Trimegestone) 19nortestosterone (Dienogest) Chlormadinone Cyproterone 17-OH Medroxyprogesterone/Medroxyprogestero ne 17-acetate# Megestrol Pregnenedione (Gestonorone) Pregnene (Ethisterone) Pregnadiene Other/ (Medrogestone Melengestrol) ungroupe Norpregnane (Norgestrienone) d Lynestrenol Norethynodrel Tibolone Dydrogesterone Quingestanol Antiprogestin antagonist: Mifepristone / Asoprisnil CDB-4124 Ulipristal acetate SPRM Diosgenin Estradiol (Ethinylestradiol#/Mestranol Estradiol 17 beta-cypionate# Steroidal Polyestradiol phosphate) Estrone (Estrone sulfate) Estriol Promestriene Equilenin Equilin

Progestogens/ progestins (progesterone )

Agonist

Estrogens

Agonist

Chlorotrianisene Dienestrol Nonsteroidal Fosfestrol Diethylstilbestrol Zeranol Afimoxifene Arzoxifene Bazedoxifene Cyclofenil Lasofoxifene Ormeloxifene Antiestrogen/ Raloxifene Tamoxifen Toremifene SERM Clomifene# Mepitiostane Nafoxidine pure antagonist: Fulvestrant nonselective: Aminoglutethimide Testolactone selective: Anastrozole Atamestane Exemestane Fadrozole Formestane Letrozole Vorozole # WHO-EM. Withdrawn from market. Clinical trials: Phase III. Never to phase III M: FRS anat/phys/devp noco/cong/npls, proc/asst, drug sysi/epon (G1/G2B/G3CD) v d eCholesterol and steroid metabolic intermediates Acetyl-CoA Acetoacetyl-CoA HMGCoA Acetone Acetoacetic acid betaKetone bodies Hydroxybutyric acid to HMG-CoA Mevalonate pathway Mevalonic acid Phosphomevalonic acid 5-Diphosphomevalonic acid Isopentenyl to DMAPP pyrophosphate Dimethylallyl pyrophosphate Geranyl pyrophosphate Geranylgeranyl Geranylpyrophosphate Carotenoid Prephytoene diphosphate Phytoene DOXP MEP CDP-ME CDP-MEP MEcPP HMBPP IPP DMAPP Farnesyl pyrophosphate Squalene 2,3-Oxidosqualene Lanosterol Lanosterol Lathosterol 7-Dehydrocholesterol Cholesterol Lanosterol Zymosterol 7-Dehydrodesmosterol Desmosterol Cholesterol Steroid Pregnenolone Corticosteroid Mineralocorticoid Progesterone s s Cortodoxone (C21 Aromatase inhibitors

Non-mevalonate pathway

To Cholesterol

pregnane)

Corticosterone Aldosterone Pregnenolone 17Hydroxypregnenolone 17Glucocorticoids Hydroxyprogesterone Cortisol Cortisol Cortisone DHEA Androstenedione/5Androstenediol Androgens Testosterone (C19 androstane) Dihydrotestosterone DHEA sulfate Epitestosterone Estrogens Estrone Estradiol (C18 estrane) Estriol

Sex steroids

Phytosterols Stigmasterol Brassicasterol Ergosterols Ergosterol Ergocalciferol M: MET mt, k, c/g/r/p/y/i, k, cgrp/y/i, f/h/s/l/o/e, m(A16/C10),i(k, f/h/s/l/o/e, a/u, n, m au, n, m, epon c/g/r/p/y/i, f/h/s/o/e, a/u, n, m) M: END anat/phys/devp/horm noco(d)/cong/tumr, proc, drug sysi/epon (A10/H1/H2/H3/H5) biochemical families: prot nucl carb (glpr, alco, glys) lipd (fata/i, phld, strd, gllp, eico) amac/i ncbs/i ttpy/i Retrieved from "http://en.wikipedia.org/w/index.php?title=Progesterone&oldid=455295515" Categories: Progestagens Neurosteroids Steroid hormones Human hormones Hormones of the hypothalamus-pituitary-adrenal axis Hormones of the hypothalamus-pituitary-gonad axis Hormones of the ovary Hormones of the placenta Hormones of the suprarenal cortex Hormones of the brain Nonhuman

Hormones of the pregnant female Hidden categories: Articles with changed KEGG identifier Drugboxes which contain changes to verified fields Drugboxes which contain changes to watched fields All articles with unsourced statements Articles with unsourced statements from November 2008
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