WordNet

a potent substance that acts like a hormone and is found in many bodily tissues (and especially in semen); produced in response to trauma and may affect blood pressure and metabolism and smooth muscle activity
the 5th letter of the Roman alphabet (同)e

Wikipedia preview

出典(authority):フリー百科事典『ウィキペディア（Wikipedia）』「2018/08/15 05:24:14」(JST)

wiki en

Prostaglandin E2 (PGE2), also known as dinoprostone, is a naturally occurring prostaglandin which is used as a medication.^[1] As a medication it is used in labor induction, bleeding after delivery, termination of pregnancy, and in newborn babies to keep the ductus arteriosus open.^[1]^[2] In babies it is used in those with congenital heart defects until surgery can be carried out.^[2] It may be used within the vagina or by injection into a vein.^[1]^[3]

Common side effects include vomiting, fever, diarrhea, and excessive uterine contraction.^[1] In babies there may be decreased breathing and low blood pressure.^[2] Care should be taken in people with asthma or glaucoma and it is not recommended in those who have had a prior C-section.^[4] Prostaglandin E2 is in the oxytocics family of medications. It works by binding and activating the prostaglandin E2 receptor which results in the opening and softening of the cervix and dilation of blood vessels.^[1]^[2]

Prostaglandin E2 was first made in 1970 and approved for medical use in the United States in 1977.^[2]^[1] It is on the World Health Organization's List of Essential Medicines, the most effective and safe medicines needed in a health system.^[5] In the United Kingdom a dose costs the NHS about 8.50 to 30.00 pounds.^[3]^[6] In the United States a course of treatment costs more than 200 USD.^[4] Prostaglandin E2 works as well as prostaglandin E1 in babies; however, it is much less expensive.^[2]

Physiological effects

It has important effects in labour (softening the cervix and causing uterine contraction) and also stimulates osteoblasts to release factors that stimulate bone resorption by osteoclasts. PGE2 is also the prostaglandin that ultimately induces fever. It is also implicated in duct-dependent congenital heart diseases and is used in infusion in order to open the duct although PGE1 is more commonly used.

It is a direct vasodilator, relaxing smooth muscles, and it inhibits the release of noradrenaline from sympathetic nerve terminals. It does not inhibit platelet aggregation, where PGI2 does.

PGE2 also suppresses T cell receptor signaling and may play a role in resolution of inflammation.^[7] Up-regulation of PGE2 has been implicated as a possible cause of nail clubbing. Furthermore, its postpartal synthesis in newborns is considered as one cause of patent ductus arteriosus.^[8]

Side effects

Common side effects include vomiting, fever, diarrhea, and excessive uterine contraction.^[1] In babies there may be decreased breathing and low blood pressure.^[2] Care should be taken in people with asthma or glaucoma and it is not recommended in those who have had a prior C-section.^[4]

Mechanism of action

PGE2 is a potent activator of the Wnt signaling pathway. It has been implicated in regulating the developmental specification and regeneration of hematopoietic stem cells through cAMP/PKA activity.^[9]

History

It was discovered by Bunting, Gryglewski, Moncada and Vane in 1976.

Society and culture

It is sold under the trade name of Cervidil(US) and Propess (by Ferring Pharmaceuticals). This is a controlled release vaginal insert. Prostin E₂ (by Pfizer Inc.), and Glandin (by Nabiqasim Pharmaceuticals Pakistan) as a vaginal suppository, to prepare the cervix for labour; it is used to induce labour.

References

^ ^a ^b ^c ^d ^e ^f ^g "Dinoprostone". The American Society of Health-System Pharmacists. Archived from the original on 16 January 2017. Retrieved 8 January 2017.
^ ^a ^b ^c ^d ^e ^f ^g Northern Neonatal Network (208). Neonatal Formulary: Drug Use in Pregnancy and the First Year of Life (5 ed.). John Wiley & Sons. p. 2010. ISBN 9780470750353. Archived from the original on 2017-01-13.
^ ^a ^b British national formulary : BNF 69 (69 ed.). British Medical Association. 2015. pp. 538–540. ISBN 9780857111562.
^ ^a ^b ^c Hamilton, Richart (2015). Tarascon Pocket Pharmacopoeia 2015 Deluxe Lab-Coat Edition. Jones & Bartlett Learning. p. 361. ISBN 9781284057560.
^ "WHO Model List of Essential Medicines (19th List)" (PDF). World Health Organization. April 2015. Archived (PDF) from the original on 13 December 2016. Retrieved 8 December 2016.
^ Ainsworth, Sean B. (2014). Neonatal Formulary: Drug Use in Pregnancy and the First Year of Life. John Wiley & Sons. p. 436. ISBN 9781118819593. Archived from the original on 2017-01-13.
^ Wiemer, AJ; Hegde, S; Gumperz, JE; Huttenlocher, A (1 October 2011). "A live imaging cell motility screen identifies prostaglandin E2 as a T cell stop signal antagonist". Journal of Immunology. 187 (7): 3663–70. doi:10.4049/jimmunol.1100103. PMC 3178752 . PMID 21900181.
^ Textbook of Pathology 7th Edition © 2015, Harsh Mohan; ISBN 978-93-5152-369-7; p. 404
^ Goessling, Wolfram; North, Trista E.; Loewer, Sabine; Lord, Allegra M.; Lee, Sang; Stoick-Cooper, Cristi L.; Weidinger, Gilbert; Puder, Mark; Daley, George Q. (2009-03-20). "Genetic interaction of PGE2 and Wnt signaling regulates developmental specification of stem cells and regeneration". Cell. 136 (6): 1136–1147. doi:10.1016/j.cell.2009.01.015. ISSN 1097-4172. PMC 2692708 . PMID 19303855.

External links

Cervidil/Prostin E2 - drugs.com

UpToDate Contents

全文を閲覧するには購読必要です。 To read the full text you will need to subscribe.

1. 早産児における動脈管開存症の病態生理、臨床症状、および診断 pathophysiology clinical manifestations and diagnosis of patent ductus arteriosus in premature infants
2. Techniques for ripening the unfavorable cervix prior to induction
3. 早産児の動脈管開存症のマネージメント management of patent ductus arteriosus in preterm infants
4. 帝王切開歴がある女性における頸管熟化および陣痛の誘発 cervical ripening and induction of labor in women with a prior cesarean delivery
5. 妊娠中期の中絶：子宮内容除去術 second trimester pregnancy termination dilation and evacuation

English Journal

Diesel and biodiesel exhaust particle effects on rat alveolar macrophages with in vitro exposure.

Bhavaraju L1, Shannahan J2, William A3, McCormick R3, McGee J4, Kodavanti U4, Madden M5.Author information 1Currciculum in Toxicology, University of North Carolina, Chapel Hill, NC, United States.2School of Pharmacy, University of Colorado, Denver, CO, United States.3National Renewable Energy Laboratory, Golden, CO, United States.4EPHD, NHEERL, US EPA, Research Triangle Park, NC, United States.5EPHD, NHEERL, US EPA, Research Triangle Park, NC, United States. Electronic address: madden.michael@epa.gov.AbstractCombustion emissions from diesel engines emit particulate matter which deposits within the lungs. Alveolar macrophages (AMs) encounter the particles and attempt to engulf the particles. Emissions particles from diesel combustion engines have been found to contain diverse biologically active components including metals and polyaromatic hydrocarbons which cause adverse health effects. However little is known about AM response to particles from the incorporation of biodiesel. The objective of this study was to examine the toxicity in Wistar Kyoto rat AM of biodiesel blend (B20) and low sulfur petroleum diesel (PDEP) exhaust particles. Particles were independently suspended in media at a range of 1-500μgmL(-1). Results indicated B20 and PDEP initiated a dose dependent increase of inflammatory signals from AM after exposure. After 24h exposure to B20 and PDEP gene expression of cyclooxygenase-2 (COX-2) and macrophage inflammatory protein 2 (MIP-2) increased. B20 exposure resulted in elevated prostaglandin E2 (PGE2) release at lower particle concentrations compared to PDEP. B20 and PDEP demonstrated similar affinity for sequestration of PGE2 at high concentrations, suggesting detection is not impaired. Our data suggests PGE2 release from AM is dependent on the chemical composition of the particles. Particle analysis including measurements of metals and ions indicate B20 contains more of select metals than PDEP. Other particle components generally reduced by 20% with 20% incorporation of biodiesel into original diesel. This study shows AM exposure to B20 results in increased production of PGE2in vitro relative to diesel.
Chemosphere.Chemosphere.2014 Jun;104:126-33. doi: 10.1016/j.chemosphere.2013.10.080. Epub 2013 Nov 21.
Combustion emissions from diesel engines emit particulate matter which deposits within the lungs. Alveolar macrophages (AMs) encounter the particles and attempt to engulf the particles. Emissions particles from diesel combustion engines have been found to contain diverse biologically active componen
PMID 24268344

Ovarian steroid-dependent tumor necrosis factor-α production and its action on the equine endometrium in vitro.

Szóstek AZ1, Adamowski M2, Galvão AM3, Ferreira-Dias GM2, Skarzynski DJ4.Author information 1Department of Reproductive Immunology and Pathology, Institute of Animal Reproduction and Food Research, Olsztyn, Poland.2C.I.I.S.A., Faculty of Veterinary Medicine, University of Lisbon, Lisbon, Portugal.3Department of Reproductive Immunology and Pathology, Institute of Animal Reproduction and Food Research, Olsztyn, Poland; C.I.I.S.A., Faculty of Veterinary Medicine, University of Lisbon, Lisbon, Portugal.4Department of Reproductive Immunology and Pathology, Institute of Animal Reproduction and Food Research, Olsztyn, Poland. Electronic address: d.skarzynski@pan.olsztyn.pl.AbstractTumor necrosis factor-α (TNF) is a cytokine that plays important roles in functions of the endometrium. The aims of this study were to determine whether (i) ovarian steroids modulate TNF production by endometrial cells (Experiment 1); (ii) TNF effects on prostaglandin (PG) production in cultured equine endometrial cells and tissue (Experiment 2). Epithelial and stromal cells were isolated from equine endometrium (Days 2-5 of the estrous cycle; n=20) and treated after passage 1. In Experiment 1, epithelial and stromal cells were exposed to progesterone (P4; 10(-7)M), 17-β estradiol (E2; 10(-9)M) or P4+E2 (10(-7)/10(-9)M) for 24h. Then, TNF mRNA transcription was determined using Real-time PCR. Additionally, TNF protein production was investigated in response to ovarian steroids for 24h using Enzyme-Linked Immunosorbent Spot (EliSpot). In Experiment 2, epithelial and stromal cells and endometrial explants (mid-luteal phase of the estrous cycle; n=5) were exposed in vitro to TNF (10ng/ml) and to oxytocin (OT; positive control; 10(-7)M) for 24h. The concentrations of PGE2 and PGF2α were determined using a direct enzyme immunoassay (EIA) method. The transcription of prostaglandin-endoperoxide synthase-2 (PTGS-2), prostaglandin E2 synthase (PGES) and PGF2α synthase (PGFS) mRNAs in the endometrial explants was determined using Real-time PCR. Results showed that TNF is produced by two types of equine endometrial cells and its production is up-regulated by ovarian steroids (P<0.05) in stromal cells and by P4 (P<0.05) and E2 (P<0.01) in epithelial cells. Epithelial and stromal cells can also produce PG in response to TNF. In endometrial explants, TNF stimulated PGE2 production to a large extent and PGF2α secretion to a lesser extent. These actions are mediated by up-regulation of PG synthases mRNA transcription. The study indicates that TNF production is closely related to ovarian steroid actions and that the interaction between TNF and PG regulates physiologic processes in the equine endometrium.
Cytokine.Cytokine.2014 Jun;67(2):85-91. doi: 10.1016/j.cyto.2014.02.005. Epub 2014 Mar 15.
Tumor necrosis factor-α (TNF) is a cytokine that plays important roles in functions of the endometrium. The aims of this study were to determine whether (i) ovarian steroids modulate TNF production by endometrial cells (Experiment 1); (ii) TNF effects on prostaglandin (PG) production in cultured eq
PMID 24642167

Intratumoral COX-2 inhibition enhances GM-CSF immunotherapy against established mouse GL261 brain tumors.

Eberstål S1, Sandén E, Fritzell S, Darabi A, Visse E, Siesjö P.Author information 1Glioma Immunotherapy Group, Division of Neurosurgery, Department of Clinical Sciences, Lund University, Lund, Sweden.AbstractImmunotherapy has shown effectiveness against experimental malignant brain tumors, but the clinical results have been less convincing most likely due to immunosuppression. Prostaglandin E2 (PGE2 ) is the key immunosuppressive product of cyclooxygenase-2 (COX-2) and increased levels of PGE2 and COX-2 have been shown in several tumor types, including brain tumors. In the current study, we report enhanced cure rate of mice with established mouse GL261 brain tumors when immunized with granulocyte macrophage-colony stimulating factor (GM-CSF) secreting tumor cells and simultaneously treated with the selective COX-2 inhibitors parecoxib systemically (5 mg/kg/day; 69% cure rate) or valdecoxib intratumorally (5.3 µg/kg/day; 63% cure rate). Both combined therapies induced a systemic antitumor response of proliferating CD4(+) and CD8(+) T cells, and further analysis revealed T helper 1 (Th 1) cell supremacy. The GL261 tumor cell line produced low levels of PGE2 in vitro, and co-staining at the tumor site demonstrated that a large fraction of the COX-2(+) cells were derived from CD45(+) immune cells and more specifically macrophages (F4/80(+)), indicating that tumor-infiltrating immune cells constitute the primary source of COX-2 and PGE2 in this model. We conclude that intratumoral COX-2 inhibition potentiates GM-CSF immunotherapy against established brain tumors at substantially lower doses than systemic administration. These findings underscore the central role of targeting COX-2 during immunotherapy and implicate intratumoral COX-2 as the primary target.
International journal of cancer. Journal international du cancer.Int J Cancer.2014 Jun 1;134(11):2748-53. doi: 10.1002/ijc.28607. Epub 2013 Nov 25.
Immunotherapy has shown effectiveness against experimental malignant brain tumors, but the clinical results have been less convincing most likely due to immunosuppression. Prostaglandin E2 (PGE2 ) is the key immunosuppressive product of cyclooxygenase-2 (COX-2) and increased levels of PGE2 and COX-2
PMID 24243648

Japanese Journal

The inflammatory network in the gastrointestinal tumor microenvironment: lessons from mouse models

Oshima Hiroko,Oshima Masanobu
Journal of Gastroenterology 47(2), 97-106, 2012-02
… Subsequently, mouse genetic studies have shown that cyclooxygenase (COX)-2, one of the target molecules of NSAIDs, and its downstream product, prostaglandin E 2 (PGE 2), play an important role in gastrointestinal tumorigenesis. …
NAID 80022322740

〈Review〉Target validation and drug discovery for in flammatory diseases

Takahashi Hideo Kohka
Acta Medica Kinki University 36(2), 45-52, 2011-12
… It is reported that monocyte/macropharge releases histamine, prostaglandin (PG)E2, interleukin (IL)-18 and high mobility group box-1 (HMGB1). …
NAID 80022302903

Related Pictures

★リンクテーブル★

リンク元	「ガルナー症候群」「dinoprostone」
拡張検索	「16,16-dimethylprostaglandin E2」
関連記事	「prostaglandin」「E2」「E」「prostaglandins」

「ガルナー症候群」

Prostaglandin E2
Clinical data
Trade names	PGE2, Cervidil, Propess, others
Synonyms	(5Z,11α,13E,15S)-11,15-Dihydroxy-9-oxo-prosta-5,13-dien-1-oic acid
AHFS/Drugs.com	Monograph
MedlinePlus	a682512
Pregnancy; category	US: C (Risk not ruled out) ; ;
Routes of; administration	intravaginal, IV
ATC code	G02AD02 (WHO) ;
Identifiers
	IUPAC name (5Z,11α,13E,15S)-7-[3-hydroxy-2-(3-hydroxyoct-1-enyl)- 5-oxo-cyclopentyl] hept-5-enoic acid;
CAS Number	363-24-6 ;
PubChem CID	5280360;
IUPHAR/BPS	1883;
DrugBank	DB00917 ;
ChemSpider	4444059 ;
ChEBI	CHEBI:15551 ;
ChEMBL	CHEMBL548 ;
ECHA InfoCard	100.006.052
Chemical and physical data
Formula	C20H32O5
Molar mass	352.465 g/mol
3D model (JSmol)	Interactive image;
	SMILES CCCCC[C@@H](/C=C/[C@H]1[C@@H](CC(=O)[C@@H]1C/C=C\CCCC(=O)O)O)O;
	InChI InChI=1S/C20H32O5/c1-2-3-6-9-15(21)12-13-17-16(18(22)14-19(17)23)10-7-4-5-8-11-20(24)25/h4,7,12-13,15-17,19,21,23H,2-3,5-6,8-11,14H2,1H3,(H,24,25)/b7-4-,13-12+/t15-,16+,17+,19+/m0/s1 ; Key:XEYBRNLFEZDVAW-ARSRFYASSA-N ;
(what is this?) (verify)

　　[★]

英: Gullner syndrome

低カリウム血性アルカローシスと腎尿細管障害を呈する症候群。
Gullner et al. (1980, 1983) studied 3 black sibs (2 girls, 1 boy) with hypokalemia. Their disorder resembled Bartter syndrome in the presence of hyperreninemia, high urinary prostaglandin E2, normal blood pressure, and resistance of BP to the pressor effect of angiotensin II. In contrast to Bartter syndrome, the juxtaglomerular apparatus was histologically normal and changes were observed in the proximal tubules: intense staining of the cells, extreme hypertrophy of the basement membranes, and, by electron microscopy, dense cytoplasm, compact mitochondria, and pyknotic nuclei. Glomerular distal tubular and loop of Henle functions were normal. The 3 affected sibs had identical HLA-A and HLA-B types whereas a single unaffected sib had the complementary haplotype. A lod score of 1.322 (21:1 odds; P less than 0.05) for linkage was calculated.(参考1)

参考

1. HYPOKALEMIA, FAMILIAL - OMIM

http://www.ncbi.nlm.nih.gov/omim?term=Gullner syndrome

「dinoprostone」

　　[★]

ジノプロストン

関: dinoprostone betadex、PGE2、prostaglandin E2

「16,16-dimethylprostaglandin E2」

　　[★]

16

関: 16,16-dimethyl-PGE2

「prostaglandin」

　　[★] プロスタグランジン prostaglandins PG

「E2」

　　[★] エストラジオール estradiol

「E」

　　[★]

「prostaglandins」

　　[★] プロスタグランジン

[AHFS2017-1] ^ ^a ^b ^c ^d ^e ^f ^g "Dinoprostone". The American Society of Health-System Pharmacists. Archived from the original on 16 January 2017. Retrieved 8 January 2017.

[No2010-2] ^ ^a ^b ^c ^d ^e ^f ^g Northern Neonatal Network (208). Neonatal Formulary: Drug Use in Pregnancy and the First Year of Life (5 ed.). John Wiley & Sons. p. 2010. ISBN 9780470750353. Archived from the original on 2017-01-13.

[BNF69-3] British national formulary : BNF 69 (69 ed.). British Medical Association. 2015. pp. 538–540. ISBN 9780857111562.

[Ric2015-4] Hamilton, Richart (2015). Tarascon Pocket Pharmacopoeia 2015 Deluxe Lab-Coat Edition. Jones & Bartlett Learning. p. 361. ISBN 9781284057560.

[WHO19th-5] "WHO Model List of Essential Medicines (19th List)" (PDF). World Health Organization. April 2015. Archived (PDF) from the original on 13 December 2016. Retrieved 8 December 2016.

[6] Ainsworth, Sean B. (2014). Neonatal Formulary: Drug Use in Pregnancy and the First Year of Life. John Wiley & Sons. p. 436. ISBN 9781118819593. Archived from the original on 2017-01-13.

[7] Wiemer, AJ; Hegde, S; Gumperz, JE; Huttenlocher, A (1 October 2011). "A live imaging cell motility screen identifies prostaglandin E2 as a T cell stop signal antagonist". Journal of Immunology. 187 (7): 3663–70. doi:10.4049/jimmunol.1100103. PMC 3178752 . PMID 21900181.

[8] Textbook of Pathology 7th Edition © 2015, Harsh Mohan; ISBN 978-93-5152-369-7; p. 404

[9] Goessling, Wolfram; North, Trista E.; Loewer, Sabine; Lord, Allegra M.; Lee, Sang; Stoick-Cooper, Cristi L.; Weidinger, Gilbert; Puder, Mark; Daley, George Q. (2009-03-20). "Genetic interaction of PGE2 and Wnt signaling regulates developmental specification of stem cells and regeneration". Cell. 136 (6): 1136–1147. doi:10.1016/j.cell.2009.01.015. ISSN 1097-4172. PMC 2692708 . PMID 19303855.

v t e Tocolytics/labor repressants (G02CA)
β₂ adrenoreceptor agonists	Buphenine Fenoterol Hexoprenaline Ritodrine Terbutaline
Oxytocin antagonists	Atosiban
NSAIDs	Indometacin
Calcium channel blockers	Nifedipine
Myosin inhibitors	Magnesium sulfate

匿名

検索

案内

案内

prostaglandin E2