Monograph
G03DA04 - Progesterone |
Probably porphyrinogenic |
PRP |
Side effects
A suggested hypothesis for the porphyrinogenic potential of progestins (Thunell 2016) is that they activate the mPRalpha-PGRMC2 receptor complex (Thomas 2013), which is accompanied by heme binding (Rohe 2009), and may therefore result in a heme drain. A decreased cellular heme pool may then upregulate ALAS-1 (Besur 2014). In addition, the heme-sensing receptor, Rev-erb-alpha, will sense the decreased level of the regulatory heme pool and reduce its repressor effect on PGC-1alpha (Wu 2009). PGC-1alpha may then co-activate FoxO1 and NRF-1, with subsequent induction of the ALAS-1 gene (Handschin 2005).
Rationale
Progesterone is considered as a potentially porphyrinogenic substance and is known to have caused porphyric attacks in susceptible carriers of acute porphyria. Both pharmacodynamic and pharmacokinetic properties can explain the triggering effect in acute porphyria. Studies have shown that this hormone can affect CYP enzymes by induction. Although this effect is described to a limited extent in drug-drug interactions studies in general, it is likely that it has a role in a probable upregulation of the heme biosynthesis.
Chemical description
Progesterone is a steroid hormone.
Therapeutic characteristics
Progesterone is used in the treatment of dysfunctional uterine bleedings, amenorrhea, for prevention of endometrial hyperplasia caused by conjugated estrogen and as part of assisted reproductive technology treatment. Progesterone may be administered by the oral, intramuscular, subcutaneous, rectal or vaginal route.
Metabolism and pharmacokinetics
Progesterone activate PXR (Kliewer 1998 Honkakoski 2003).
Progesterone is not listed as a significant inducer of CYP 3A4 in most interaction databases (Preissner 2010, NOMA, Lexi-Interact, The Danish Healt and Medicines Authority, Micromedex).
Results from clinical studies suggest that the increased hormonal levels in pregnancy have the potential to alter hepatic cytochrome P450 drug metabolism (Anderson 2005). Also, in vitro studies have shown increased CYP mRNA after exposing hepatocytes to progesterone and estradiol levels equal to the high hormonal levels typically seen in the third trimester of pregnancy (Choi 2013).
Hormonal therapy generally leads to a much lower plasma concentration relative to the levels of endogenous hormones in pregnancy and may explain the lack of observed significant effects of administered hormones on CYP 3A4 in vivo.
Studies have shown that women with acute porphyria have an altered 5 alpha-reductase steroid metabolism and it is suggested that this may lead to a diversion from the 5 alpha reductase pathway to formation of 5beta steroid metabolites that may be more potent inductors of ALAS1 (Innala 2012, Anderson 1979, Jacobs 2005).
Preclinical data
It is from clinical observations well known that progestogens have a role in precipitating acute porphyric attacks (Andersson 2003, Kauppinen 1992, Bonkovsky 2014).
IPNet drug reports
One report of an attack requiring hospitalisation in a 31 year-old susceptible female with AIP. However there were other factors that could have contributed to the attack. Uneventful use reported in 11 patients with acute porphyria.
Similar drugs
References
| # | Citation details | PMID |
|---|---|---|
| * | Scientific articles | |
| 1. | Pregnancy-induced changes in pharmacokinetics: a mechanistic-based approach.
Anderson GD. Clin Pharmacokinet. 2005;44(10):989-1008. |
16176115 |
| 2. | Studies in porphyria. VIII. Relationship of the 5 alpha-reductive metabolism of steroid hormones to clinical expression of the genetic defect in acute intermittent porphyria.
Anderson KE, Bradlow HL, et al. Am J Med. 1979 Apr;66(4):644-50. |
433969 |
| 3. | Acute intermittent porphyria in women: clinical expression, use and experience of exogenous sex hormones. A population-based study in northern Sweden.
Andersson C, Innala E, et al. J Intern Med. 2003 Aug;254(2):176-83. |
12859699 |
| 4. | Clinically important features of porphyrin and heme metabolism and the porphyrias.
Besur S, Hou W, et al. Metabolites. 2014 Nov 3;4(4):977-1006. |
|
| 5. | Acute porphyrias in the USA: features of 108 subjects from porphyrias consortium.
Bonkovsky HL, Maddukuri VC et al. Am J Med. 2014 Dec;127(12):1233-41 |
25016127 |
| 6. | Isoform-specific regulation of cytochrome P450 expression by estradiol and progesterone. Drug Metab Dispos 2013 Feb. 41:253-269.
Choi S-Y, Koh KH, et al. |
|
| 7. | Nutritional regulation of hepatic heme biosynthesis and porphyria through PGC-1alpha.
Handschin C, Lin J, et al. Cell. 2005 Aug 26;122(4):505-15. |
16122419 |
| 8. | Drug-activated nuclear receptors CAR and PXR.
Honkakoski P, Sueyoshi T, et al. Ann Med. 2003;35(3):172-82. |
|
| 9. | Women with acute intermittent porphyria have a defect in 5alpha-steroid production during the menstrual cycle.
Innala E, Bäckström T et al. Acta Obstet Gynecol Scand. 2012 Dec;91(12):1445-52. |
22924787 |
| 10. | Lignans, bacteriocides and organochlorine compounds activate the human pregnane X receptor (PXR).
Jacobs MN, Nolan GT, et al. Toxicol Appl Pharmacol. 2005 Dec 1;209(2):123-33. |
15885729 |
| 11. | Prognosis of acute porphyria: occurrence of acute attacks, precipitating factors, and associated diseases. Medicine (Baltimore). 1992 Jan;71(1):1-13.
Kauppinen R, Mustajoki P. |
1549056 |
| 12. | An orphan nuclear receptor activated by pregnanes defines a novel steroid signaling pathway.
Kliewer SA, Moore JT, et al. Cell. 1998 Jan 9;92(1):73-82. |
9489701 |
| 13. | SuperCYP: a comprehensive database on Cytochrome P450 enzymes including a tool for analysis of CYP-drug interactions.
Preissner S, Kroll K, et al. Nucleic Acids Res. 2010 Jan;38(Database issue):D237-43. |
19934256 |
| 14. | PGRMC1 (progesterone receptor membrane component 1): a targetable protein with multiple functions in steroid signaling, P450 activation and drug binding.
Rohe HJ, Ahmed IS, et al. Pharmacol Ther. 2009 Jan;121(1):14-9. |
18992768 |
| 15. | Enhancement of cell surface expression and receptor functions of membrane progestin receptor alpha (mPRalpha by progesterone receptor membrane component 1 (PGRMC1): evidence for a role of PGRMC1 as an adaptor protein for steroid receptors.
Thomas P, Pang Y, et al. Endocrinology. 2014 Mar;155(3):1107-19. |
24424068 |
| 16. | Genetik och metabola förlopp bakom den akuta porfyriattacken - Mer än hundra läkemedel är potentiellt livshotande vid akut porfyri.
Thunell S. Lakartidningen. 2016 Sep 9;113. |
|
| 17. | Negative feedback maintenance of heme homeostasis by its receptor, Rev-erb-alpha.
Wu N, Yin L, et al. Genes Dev. 2009 Sep 15;23(18):2201-9 |
|
| * | Government bodies | |
| 18. | Norwegian medicines agency (NOMA). Find medicine.
|
|
| * | Drug interaction databases | |
| 19. | Lexi-Interact, via UpToDate.
|
|
| 20. | Micromedex® 2.0 (online). Drug Interactions). (23.08.2017).
|
|
| * | Summary of Product Characteristics | |
| 21. | The electronic Medicines Compendium (emc). Summary of Product Characteristics (SPC). Utrogestan.
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Tradenames
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Consequently, very similar terms may therefore appear multiple times.
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Crinone 80 mg/g gel voor vaginaal gebruik · Cyclogest 400 mg, ovule · Lutinus 100 mg, tabletten voor vaginaal gebruik · Progesteron Besins 100 mg zachte capsules · Progesteron Besins 200 mg zachte capsules · Progesteron ERC 100 mg, zachte capsules · Prolutex 25 mg, oplossing voor injectie · Prolutex 25 mg, oplossing voor injectie in een voorgevulde spuit · Utrogestan 200 mg, zachte capsules voor vaginaal gebruik · Utrogestan 300 mg, zachte capsules voor vaginaal gebruik · Utrogestan 400 mg, zachte capsules voor vaginaal gebruik · Utrogestan, capsules 100 mg 
Amelgen 400 mg ovule · Crinone 8 % gel vagin. · Gepretix 100 mg caps. molle · Gepretix 200 mg caps. molle · Inprosub · Inprosub 25 mg sol. inj. s.c. ser. pr?remplie · Inprosub 25 mg sol. inj. s.c./i.m. flac. · Progebel 100 mg caps. molle · Progebel 200 mg caps. molle · Progesteron Besins 100 mg caps. molle · Progesteron Besins 200 mg caps. molle · Progestogel 1 % 1 % gel · Utrogestan 100 mg caps. molle · Utrogestan 200 mg caps. molle · Utrogestan Vaginal 100 mg caps. molle · Utrogestan Vaginal 200 mg caps. molle · Utrogestan Vaginal 300 mg caps. molle · Utrogestan Vaginal 400 mg caps. molle vagin. 
Crinone 8% gel Vaginal · Cyclogest 400 mg Ovulos · DARSTIN 10 mg/g GEL · Gepretix 100 mg Capsulas Blandas efg · Gepretix 200 mg Capsulas Blandas efg · PROGEFFIK 100 mg CAPSULAS BLANDAS · Progeffik 200 mg Capsulas Blandas · Prolutex 25 mg Solucion Inyectable · Prolutex 25 mg Solucion Inyectable en Jeringa Precargada · Seidigestan · SEIDIGESTAN 100 mg c?psulas blandas · SEIDIGESTAN 200 mg c?psulas blandas · Utrogestan 200 mg Capsulas Vaginales Blandas · Utrogestan 300 mg Capsulas Vaginales Blandas 
Amelgen · Crinone · Progeffik · Prometrium · Prontogest 
AREFAM 200 mg · CRINONE 80 mg/g · CYCLOVITA 400 mg · LUTINUS 100 mg · MASTOPROFEN 10 mg/g · PROLUTEX 25 mg · UTROGESTAN 100 mg · UTROGESTAN 200 mg 
Crinone 4% progesterone · Crinone 8% progesterone · Cyclogest · Gepretix · Gestone · Lubion · Lutigest · Pro-Juven · Progesterone · Prontogest · Serenity Progesterone · Utrogestan 
Amelgen · Crinone · Cyclogest · Lutinus · Pleyris · Progestan · Prolutex · Utrogestan 
Crinone · Cyclogest · Gepretix · Lutinus · Progeffik · Progestan · Progesteron SA · Prolutex · Utrogest · Utrogestan 
Crinone · Cyclogest · Famenita · Lustork · Luteina · Luteina 50 · Lutezin · Lutinus · Luttagen · Progesteron Adamed · Progesterone Besins · Prolutex · Utrogestan 
Amelgen · Crinone · Inprosub · Progebel · Progesteron Besins · Progestogel · Utrogestan · Utrogestan Vaginal 
Crinone · Cyclogest · Lutinus · Progestan · Progesterone Alvogen · Utrogestan 
Crinone · Cyclogest · Gepretix · Lugesteron · Lutinus · Prolutex 
Amelgen · Crinone · Gepretix · Lubion · Pleyris · Progesterone Besins · Utrogest · Utrogestan 
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