- 17-Hydroxyprogesterone
drugbox
IUPAC_name = 17-Hydroxypregn-4-ene-3,20-dione
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DrugBank =
C=21 | H=30 | O=3
molecular_weight = 330.22
melting_point = 219-220
bioavailability =
protein_bound =
metabolism =Liver
elimination_half-life =
excretion =
pregnancy_AU =
pregnancy_US =
pregnancy_category= B
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routes_of_administration = Intramuscular17-Hydroxyprogesterone (17-OH progesterone or 17OHP) is a C-21
steroid hormone produced during the synthesis ofglucocorticoid s andsex steroid s.As a hormone, 17OHP also interacts with the
progesterone receptor .Production
It is derived from
progesterone via17-hydroxylase , a P450c17 enzyme, or from17-hydroxypregnenolone via 3β-hydroxysteroid dehydrogenase/Δ5-4 isomerase.17-Hydroxyprogesterone is a natural progestin, and in pregnancy increases in the third trimester primarily due to fetal adrenal production.
This hormone is primarily produced in the
adrenal gland s and to some degree in thegonad s, specifically thecorpus luteum of theovary . Normal levels are 3-90 ng/dl in children, and in women, 15-70 ng/dl prior to ovulation, and 35-290 ng/dl during theluteal phase .17-hydroxyprogesterone caproate
17-Hydroxyprogesterone is not the same compound as 17-hydroxyprogesterone
caproate . 17-Hydroxyprogesterone caproate is a synthetic (artificial) hormone that is similar in structure tomedroxyprogesterone acetate andmegestrol acetate .The terminology is confusing because 17P is used to refer to both the natural hormone and the artificial/synthetic hormone. It is preferable to refer to the synthetic hormone as 17-OHPC.
Clinical use
Measurements of levels of 17-hydroxyprogesterone are useful in the evaluation of patients with suspected
congenital adrenal hyperplasia as the typical enzymes that are defective, namely 21-hydroxylase and 11β-hydroxylase, lead to a build-up of 17OHP. In contrast, the rare patient with 17α-hydroxylase deficiency will have very low or undetectable levels of 17OHP. 17OHP levels can also be used to measure contribution of progestational activity of the corpus luteum during pregnancy as progesterone but not 17OHP is also contributed by theplacenta .The application of 17OHP has been shown to be useful to delay
premature labor in pregnancy.Yemini M, Borenstein R, Dreazen, et al. "Prevention of premature labor by 17 alpha-hydroxyprogesterone caproate." Am J Obstet Gynecol. 1985;151(5):574-7.PMID 3976757.] Meis PJ; Society for Maternal-Fetal Medicine. "17 hydroxyprogesterone for the prevention of preterm delivery." Obstet Gynecol. 2005;105:1128-35.PMID 15863556.]The use of 17-hydroxyprogesterone caproate in pregnancy to prevent preterm birth is not recommended without further study according to two authorities. A 2006 Cochrane Review concluded "...important maternal and infant outcomes have been poorly reported to date... information regarding the potential harms of progesterone therapy to prevent preterm birth is limited". [ Dodd JM, Flenady V, Cincotta R, Crowther CA; The Cochrane Database of Systematic Reviews 2006 Issue 1] There was a similar conclusion from a review by Marc Keirse. [Keirse MJNC. Progesterone and Preterm: Seventy Years of "Deja vu" or "Still To Be Seen"?. Birth, 2004 September; 31:3.] Three clinical studies of 250 mg/week of i.m. 17-hydroxyprogesterone caproate have all shown a trend for an increase in pregnancy loss due to miscarriage compared to placebo. [Johnson JWC, Austin KL, Jones GS, Davis GH, King TM. Efficacy of 17 alpha-hydroxyprogesterone caproate in the prevention of premature labor. NEJM 1975 October. 293(14):675.] [Yemini M, Borenstein R, Dreazen, et al. Prevention of premature labor by 17 alpha-hydroxyprogesterone caproate. Am J Obstet Gynecol. 1985;151(5):574-7. ] [Meis PJ et al. Prevention of Recurrent Preterm Delivery by 17 Alpha-hydroxyprogesterone Caproate. NEJM, 2003: vol 348, no 24, pg 2379-2385.] [Keirse MJNC, Progestogen administration in pregnancy may prevent preterm delivery. Br J Obstet Gynecol 1990 February; 97:149.] There has also been a study in rhesus monkeys in which all rhesus fetuses exposed to 1 and 10 times the human dose equivalent of 17-hydroxyprogesterone caproate died in utero. [Hendrix AG, et al. Embriotoxicity of sex steroidal hormones in nonhuman primates: II. Hydroxyprogesterone caproate, estradiol valerate. Teratology 1987 February. 35 (1): 129.] Currently, 17-hydroxyprogesterone caproate is a category D progestin according to the FDA (evidence of fetal harm). There is speculation that the castor oil in the 17-hydroxyprogesterone caproate formulation may not be beneficial for pregnancy. [Duke University Medical Center, New England Journal of Medicine, correspondence, vol 349.] [Hauth JC, Gilstrap LC, Brekken AL, Hauth JM. The effect of 17 alpha-hydroxyprogesterone caproate on pregnancy outcome in an active-duty military population. Am J Obstet Gynecol. 1983 May; 146(2): 187.]
Determination
Earlier immunoassays like RIA (
radioimmunoassay ) or IRMA (immunoradiometricassay) were used to clinically determine 17-Hydroxyprogesterone. Today more sophisticated methods use gas orliquid chromatography andmass spectrometry (e.g. LC-MS/MS) [Use of Ozone Depleting Substances in Laboratories. Temanord 2003:516. http://www.norden.org/pub/ebook/2003-516.pdf] [Ohjekirja 2007 (In Finnish). HUSLAB - The laboratory of Helsinki University Central Hospital. http://www.huslab.fi/ohjekirja/] .
=AdditionalReferences
External links
* [http://redpoll.pharmacy.ualberta.ca/~aguo/www_hmdb_ca/HMDB/scripts/CCMD_HTML.cgi?METABOCARD=HMDB00374 Chemical database at ualberta.ca]
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