Cortisone: Difference between revisions
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{{Short description|Corticosteroid precursor and metabolite of cortisol}} |
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{{distinguish|cortisol}} |
{{distinguish|cortisol}} |
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| verifiedrevid = 456660597 |
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| pronounce |
| pronounce = {{IPAc-en|ˈ|k|ɔːr|t|ᵻ|s|oʊ|n}}, {{IPAc-en|ˈ|k|ɔːr|t|ᵻ|z|oʊ|n}} |
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| ImageFile1 = {{wikidata|property|raw|P117}} |
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| ImageFile = Cortison.svg |
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| ImageFile2 = {{wikidata|property|raw|P8224}} |
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| ImageFile1 = Cortisone-3D-balls.png |
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| IUPACName = 17α,21-Dihydroxypregn-4-ene-3,11,20-trione |
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| SystematicName = (1''R'',3a''S'',3b''S'',9a''R'',9b''S'',11a''S'')-1-Hydroxy-1-(hydroxyacetyl)-9a,11a-dimethyl-2,3,3a,3b,4,5,8,9,9a,9b,11,11a-dodecahydro-7''H''-cyclopenta[''a'']phenanthrene-7,10(1''H'')-dione |
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| OtherNames = |
| OtherNames = 17α,21-Dihydroxy-11-ketoprogesterone; 17α-Hydroxy-11-dehydrocorticosterone |
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| UNII_Ref = {{fdacite| |
| UNII_Ref = {{fdacite|correct|FDA}} |
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| UNII = V27W9254FZ |
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| IUPHAR_ligand = 5171 |
| IUPHAR_ligand = 5171 |
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| ChEMBL_Ref = {{ebicite|changed|EBI}} |
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'''Cortisone''' is a [[pregnene]] (21-carbon) [[steroid hormone]]. It is a naturally-occurring [[corticosteroid]] metabolite that is also used as a pharmaceutical [[prodrug]]. [[Cortisol]] is converted by the action of the enzyme [[corticosteroid 11-beta-dehydrogenase isozyme 2]] into the inactive metabolite cortisone, particularly in the kidneys. This is done by [[oxidizing]] the alcohol group at carbon 11 (in the six-membered ring fused to the five-membered ring). Cortisone is converted back to the active steroid cortisol by [[stereospecific]] [[hydrogenation]] at carbon 11 by the enzyme [[11β-Hydroxysteroid dehydrogenase type 1]], particularly in the liver. |
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⚫ | |||
The term "cortisone" is frequently misused to mean either any [[corticosteroid]] or [[hydrocortisone]], which is in fact [[cortisol]]. Many who speak of receiving a "cortisone shot" or taking "cortisone" are more likely receiving hydrocortisone or one of many other, much more potent synthetic corticosteroids. |
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<!-- Society and culture --> |
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It was first described in 1949.<ref name=Fis2006>{{cite book |last1=Fischer |first1=Jnos |last2=Ganellin |first2=C. Robin |title=Analogue-based Drug Discovery |date=2006 |publisher=John Wiley & Sons |isbn=9783527607495 |page=484 |url=https://books.google.ca/books?id=FjKfqkaKkAAC&pg=PA484 |language=en}}</ref> |
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⚫ | Cortisone can be administered as a prodrug, meaning it has to be converted by the body (specifically the liver, converting it into cortisol) after administration to be effective. It is used to treat a variety of ailments and can be administered [[intravenous]]ly, [[oral administration|oral]]ly, [[intra-articular]]ly (into a joint), or [[Transdermal|transcutaneous]]ly. Cortisone suppresses various elements of the immune system, thus reducing inflammation and attendant pain and swelling. Risks exist, in particular in the long-term use of cortisone.<ref name=mayo>{{cite web|url=http://www.mayoclinic.com/health/cortisone-shots/MY00268 |title=Cortisone shots |publisher=MayoClinic.com |date=2010-11-16 |access-date=July 31, 2013}}</ref><ref name=mayorisk2>{{cite web|url=https://www.mayoclinic.org/steroids/art-20045692 |title=Prednisone and other corticosteroids: Balance the risks and benefits |publisher=MayoClinic.com |date=2010-06-05 |access-date=2017-12-21}}</ref> However, using cortisone only results in very mild activity, and very often more potent steroids are used instead. |
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==Effects and uses== |
==Effects and uses== |
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Cortisone itself is inactive.<ref>{{cite book |editor1-last= Martindale |editor1-first= William |editor2-last= Reynolds |editor2-first= James |date=1993 |title= Martindale, The Extra Pharmacopoeia |edition=30th|publisher= Pharmaceutical Press |page=726 |isbn= 978-0853693000}}</ref> It must be converted to cortisol by the action of [[11β-hydroxysteroid dehydrogenase type 1]].<ref name="Cooper">{{cite journal |vauthors= Cooper MS, Stewart PM |date=2009 |title= 11Beta-hydroxysteroid dehydrogenase type 1 and its role in the hypothalamus-pituitary-adrenal axis, metabolic syndrome, and inflammation |journal= J Clin Endocrinol Metab |volume=94 |issue=12 |pages= 4645–4654 |doi=10.1210/jc.2009-1412 |pmid= 19837912|doi-access= free }}</ref> This primarily happens in the liver, the main site at which cortisone becomes cortisol after oral or systemic injection, and can thus have a pharmacological effect. After application to the skin or injection into a joint, local cells that express 11β-hydroxysteroid dehydrogenase type 1 instead convert it to active cortisol. |
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Cortisone, a [[glucocorticoid]], and [[Adrenaline|epinephrine]] (adrenaline) are the main substances released by the body as a reaction to stress. They elevate blood pressure and prepare the body for a [[fight or flight response]]. |
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A cortisone injection |
A cortisone injection may provide short-term pain relief and may reduce the swelling from [[inflammation]] of a [[joint]], [[tendon]], or [[bursa (anatomy)|bursa]] in, for example, the joints of the [[knee]], [[elbow]] and [[shoulder]]<ref name=mayo/> and into a broken [[coccyx]].<ref>{{cite web|url=http://www.coccyx.org/treatmen/inflamm.htm|title=injections and needles for coccyx pain|website=www.coccyx.org}}</ref> |
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⚫ | Cortisone is used by [[dermatologist]]s to treat [[keloid]]s,<ref>{{cite journal | pmid = 1582609 | year = 1992 | last1 = Zanon | first1 = E | last2 = Jungwirth | first2 = W | last3 = Anderl | first3 = H | title = Cortisone jet injection as therapy of hypertrophic keloids | volume = 24 | issue = 2 | pages = 100–2 | journal = Handchirurgie, Mikrochirurgie, Plastische Chirurgie}}</ref> relieve the symptoms of [[eczema]] and [[atopic dermatitis]],<ref>{{cite web | url = http://www.nationaleczema.org/living-with-eczema/all-about-atopic-dermatitis | title = All About Atopic Dermatitis | publisher = National Eczema Association | access-date = 2013-05-07 | archive-date = 2012-01-30 | archive-url = https://web.archive.org/web/20120130050716/http://www.nationaleczema.org/living-with-eczema/all-about-atopic-dermatitis | url-status = dead }}</ref> and stop the development of [[sarcoidosis]].<ref>{{Cite journal |url=https://www.sciencedirect.com/science/article/pii/S0096021715323463 |title=Cortisone Treatment of Sarcoidosis |year=1954 |doi=10.1378/chest.26.2.224 |last1=Bogart |first1=A.S. |last2=Daniel |first2=D.D. |last3=Poster |first3=K.G. |journal=Diseases of the Chest |volume=26 |issue=2 |pages=224–228 |pmid=13182965 }}</ref> |
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Cortisone may also be used to deliberately suppress immune response in persons with [[autoimmune disease]]s or following an [[organ transplant]] to prevent [[transplant rejection]].{{medcn|date=October 2019}} The suppression of the immune system may also be important in the treatment of inflammatory conditions.<ref>{{cite web |first1=Catherine |last1=Driver |first2=William |last2=Shiel |title=Cortisone Injection (Corticosteroid Injection) of Soft Tissues & Joints |publisher=MedicineNet.com |url=http://www.medicinenet.com/cortisone_injection/article.htm |accessdate=August 7, 2013}}</ref> |
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⚫ | Cortisone is |
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==Side effects== |
==Side effects== |
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Oral use of cortisone has a number of potential systemic |
Oral use of cortisone has a number of potential systemic adverse effects, including [[asthma]], [[hyperglycemia]], [[insulin resistance]], [[diabetes mellitus]], [[osteoporosis]], [[anxiety]], [[Depression (mood)|depression]], [[amenorrhoea]], [[cataracts]], [[glaucoma]], [[Cushing's syndrome]], [[immunosuppression|increased risk of infections]], and [[stunted growth|impaired growth]].<ref name=mayo/><ref name=mayorisk2/> With [[topical application]], it can lead to thinning of the skin, impaired [[wound healing]], [[hyperpigmentation|increased skin pigmentation]], [[tendon rupture]], and [[skin infection]]s (including [[abscesses]]).<ref>{{cite journal|last=Cole|first=BJ|author2=Schumacher |title=Injectable Corticosteroids in Modern Practice|journal= Journal of the American Academy of Orthopaedic Surgeons|date=Jan–Feb 2005|volume=13|issue=1|pages=37–46|doi=10.5435/00124635-200501000-00006|pmid=15712981|citeseerx=10.1.1.562.1931|s2cid=18658724}}</ref> |
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Local side effects are rare but can include: pain, infection, skin pigment changes, loss of fatty tissue, and tendon rupture.<ref>{{cite journal|last=Cole|first=BJ|author2=Schumacher |title=Injectable Corticosteroids in Modern Practice|journal= Journal of the American Academy of Orthopaedic Surgeons|date=Jan–Feb 2005|volume=13|pages=37–46|doi=10.5435/00124635-200501000-00006|pmid=15712981|citeseerx=10.1.1.562.1931}}</ref> |
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==History== |
==History== |
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Cortisone was first identified by the American chemists [[Edward Calvin Kendall]] and |
Cortisone was first identified by the American chemists [[Edward Calvin Kendall]] and Harold L. Mason while researching at the [[Mayo Clinic]].<ref name="urlCortisone Discovery and the Nobel Prize">{{cite web |url=http://www.mayoclinic.org/tradition-heritage/cortisone-discovery.html |title=Cortisone Discovery and the Nobel Prize |website=[[Mayo Clinic]] |access-date=2009-07-04}}</ref><ref name="Ingle">"I Went to See the Elephant" autobiography of [[Dwight Ingle|Dwight J. Ingle]], published by Vantage Press (1963), pg 94, 109</ref><ref name="Mason/Myers/Kendall">{{cite journal|url=http://www.jbc.org/content/114/3/613.full.pdf|journal=J. Biol. Chem.|volume=114|page=613 |title=The chemistry of crystalline substances isolated from the suprarenal gland|year=1936|doi=10.1016/S0021-9258(18)74790-X|access-date=2014-09-07|last1=Mason|first1=Harold L.|last2=Myers|first2=Charles S.|last3=Kendall|first3=Edward C.|issue=3|doi-access=free}}</ref> During the discovery process, cortisone was known as compound E (while [[cortisol]] was known as compound F). |
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In 1949, [[Philip S. Hench]] and colleagues discovered that large doses of injected cortisone were effective in the treatment of patients with severe [[rheumatoid arthritis]].<ref name="LemkeWilliams2008">{{cite book|author1=Thomas L. Lemke|author2=David A. Williams|title=Foye's Principles of Medicinal Chemistry|url=https://archive.org/details/foyesprinciplesm00lemk|url-access=limited|year=2008|publisher=Lippincott Williams & Wilkins|isbn=978-0-7817-6879-5|pages=[https://archive.org/details/foyesprinciplesm00lemk/page/n2289 889]–}}</ref> Kendall was awarded the 1950 [[Nobel Prize for Physiology or Medicine]] along with [[Philip Showalter Hench]] and [[Tadeusz Reichstein]] for the discovery of the structure and function of [[adrenal cortex]] hormones including cortisone.<ref>{{cite web |url=https://www.nobelprize.org/prizes/medicine/1950/summary/ |title=The Nobel Prize in Physiology or Medicine 1950 |author=<!--Not stated--> |date=2021 |website=The Nobel Prize |publisher=The Nobel Foundation |access-date=2 April 2021 |quote=}}</ref><ref>{{cite journal |last1=Glyn |first1=J|date=1998 |title= The discovery and early use of cortisone|journal= J R Soc Med |volume=91 |issue=10 |pages=513–517 |doi=10.1177/014107689809101004 |pmc= 1296908 |pmid= 10070369 }}</ref> Both Reichstein and the team of O. Wintersteiner and J. Pfiffner had separately isolated the compound prior to the discovery made by Mason and Kendall, but failed to recognize its biological significance.<ref name="Ingle"/> Mason's contributions to the crystallization and characterization of the compound have generally been forgotten outside of the Mayo Clinic.<ref name="Ingle"/> |
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⚫ | Cortisone was first produced commercially by [[Merck & Co.]] in 1948 or 1949.<ref name="LemkeWilliams2008" /><ref name="pmid13875857">{{cite journal | vauthors = Calvert DN | title = Anti-inflammatory steroids | journal = Wis. Med. J. | volume = 61 |
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⚫ | Cortisone was first produced commercially by [[Merck & Co.]] in 1948 or 1949.<ref name="LemkeWilliams2008" /><ref name="pmid13875857">{{cite journal | vauthors = Calvert DN | title = Anti-inflammatory steroids | journal = Wis. Med. J. | volume = 61 | pages = 403–4 | year = 1962 | pmid = 13875857 }}</ref> On September 30, 1949, [[Percy Lavon Julian|Percy Julian]] announced an improvement in the process of producing cortisone from [[bile acid]]s.<ref>{{cite news |last=Gibbons |first=Ray |date=1949 |title= Science gets synthetic key to rare drug; discovery is made in Chicago |work=Chicago Tribune |location=Chicago |page= 1}}</ref> This eliminated the need to use [[osmium tetroxide]], a rare, expensive, and dangerous chemical. In the UK in the early 1950s, [[John Cornforth]] and [[Kenneth Callow]] at the [[National Institute for Medical Research]] collaborated with [[Glaxo]] to produce cortisone from [[hecogenin]] from [[sisal]] plants.<ref>{{cite journal | doi = 10.1016/j.shpsc.2005.09.001 | pmid = 16337555 | title = Making British Cortisone: Glaxo and the development of Corticosteroids in Britain in the 1950s–1960s | year = 2005 | last1 = Quirke | first1 = Viviane | journal = Studies in History and Philosophy of Science Part C | volume = 36 | issue = 4 | pages = 645–674 }}</ref> |
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==Production== |
==Production== |
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Cortisone is one of several end-products of a process called [[steroidogenesis]]. This process starts with the synthesis of [[cholesterol]], which then proceeds through a series of modifications in the [[adrenal gland]] |
Cortisone is one of several end-products of a process called [[steroidogenesis]]. This process starts with the synthesis of [[cholesterol]], which then proceeds through a series of modifications in the [[adrenal gland]] to become any one of many steroid hormones. One end-product of this pathway is [[cortisol]]. For cortisol to be released from the adrenal gland, a cascade of signaling occurs. [[Corticotropin-releasing hormone]] released from the [[hypothalamus]] stimulates corticotrophs in the [[anterior pituitary]] to release [[ACTH]], which relays the signal to the adrenal cortex. Here, the [[zona fasciculata]] and [[zona reticularis]], in response to ACTH, secrete glucocorticoids, in particular cortisol. In various peripheral tissues, notably the kidneys, cortisol is inactivated to cortisone by the [[enzyme]] [[corticosteroid 11-beta-dehydrogenase isozyme 2]]. This is crucial because cortisol is a potent [[mineralocorticoid]] and would cause havoc with electrolyte levels (raising blood sodium and lowering blood potassium levels) and raise blood pressure if it were not inactivated in the kidneys.<ref name ="Cooper"/> |
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Because cortisone must be converted to cortisol before being active as a [[glucocorticoid]], its activity is less than simply administering cortisol directly (80–90%).<ref>{{Cite journal|title=Corticosteroid Dose Equivalents|url=http://emedicine.medscape.com/article/2172042-overview|journal=Medscape|access-date=20 December 2016}}</ref> |
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==Popular culture== |
==Popular culture== |
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Abuse and addiction to cortisone was the subject of the 1956 motion picture ''[[Bigger Than Life]]'', produced by and starring [[James Mason]]. Though it was a box-office flop upon its initial release,{{sfn|Cossar|2011|p=273}} many modern critics hail the film as a masterpiece and brilliant indictment of contemporary attitudes toward mental illness and addiction.{{sfn|Halliwell|2013|pp=159-162}} In 1963, [[Jean-Luc Godard]] named it one of the ten greatest American sound films ever made.<ref name=godard>{{cite web |url=http://www.openculture.com/2013/12/a-young-jean-luc-godard-picks-the-best-american-films-1963.html |title=A Young Jean-Luc Godard Picks the 10 Best American Films Ever Made (1963) |publisher=Open Culture |date=December 2, 2013 |last=Marshall |first=Colin}}</ref> |
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[[John F. Kennedy]] |
[[John F. Kennedy]] was regularly administered [[corticosteroid]]s such as cortisone as a treatment for [[Addison's disease]].<ref name=Kennedy>{{cite web |url=https://www.nytimes.com/1992/10/06/health/the-doctor-s-world-disturbing-issue-of-kennedy-s-secret-illness.html?pagewanted=all |title=The doctor's world; Disturbing Issue of Kennedy's Secret Illness |work=[[The New York Times]] |date=October 6, 1992 |last=Altman |first=Lawrence}}</ref> |
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==See also == |
==See also == |
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* [[Central serous retinopathy]] |
* [[Central serous retinopathy]] |
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* [[Corticosterol]] |
* [[Corticosterol]] |
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==External links== |
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* {{commonscat-inline}} |
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==Notes== |
==Notes== |
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{{reflist|30em}} |
{{reflist|30em}} |
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| pages=321–381 |
| pages=321–381 |
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| volume=13 |display-authors=etal}} |
| volume=13 |display-authors=etal}} |
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* {{cite book |last=Cossar |first=Harper |title=Letterboxed: The Evolution of Widescreen Cinema |year=2011 |publisher=[[University Press of Kentucky]] |isbn=978-0-813-12651-7 |url=https://books.google.com/books?id=ql1mQBeuPBsC}} |
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* {{cite book |last=Halliwell |first=Martin |title=Therapeutic Revolutions: Medicine, Psychiatry, and American Culture, 1945-1970 |year=2013 |publisher=[[Rutgers University Press]] |isbn=978-0-813-56066-3 |url=https://books.google.com/books?id=lXMRAAAAQBAJ}} |
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* {{cite journal |author=Ingle DJ |title=The biologic properties of cortisone: a review |journal=J. Clin. Endocrinol. Metab. |volume=10 |issue=10 |pages=1312–54 |date=October 1950 |pmid=14794756 |doi=10.1210/jcem-10-10-1312 |url=http://jcem.endojournals.org/cgi/pmidlookup?view=long&pmid=14794756 }}{{Dead link|date=July 2019 |bot=InternetArchiveBot |fix-attempted=yes }} |
* {{cite journal |author=Ingle DJ |title=The biologic properties of cortisone: a review |journal=J. Clin. Endocrinol. Metab. |volume=10 |issue=10 |pages=1312–54 |date=October 1950 |pmid=14794756 |doi=10.1210/jcem-10-10-1312 |url=http://jcem.endojournals.org/cgi/pmidlookup?view=long&pmid=14794756 }}{{Dead link|date=July 2019 |bot=InternetArchiveBot |fix-attempted=yes }} |
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*{{cite journal |
*{{cite journal |
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| volume=73 |
| volume=73 |
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| doi=10.1021/ja01152a551 |
| doi=10.1021/ja01152a551 |
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| issue= 8 }} |
| issue= 8 |bibcode=1951JAChS..73.4057W }} |
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{{Hormones}} |
{{Hormones}} |
Latest revision as of 05:15, 9 December 2024
Names | |
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Pronunciation | /ˈkɔːrtɪsoʊn/, /ˈkɔːrtɪzoʊn/ |
IUPAC name
17α,21-Dihydroxypregn-4-ene-3,11,20-trione
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Systematic IUPAC name
(1R,3aS,3bS,9aR,9bS,11aS)-1-Hydroxy-1-(hydroxyacetyl)-9a,11a-dimethyl-2,3,3a,3b,4,5,8,9,9a,9b,11,11a-dodecahydro-7H-cyclopenta[a]phenanthrene-7,10(1H)-dione | |
Other names
17α,21-Dihydroxy-11-ketoprogesterone; 17α-Hydroxy-11-dehydrocorticosterone
| |
Identifiers | |
3D model (JSmol)
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|
ChEBI | |
ChEMBL | |
ChemSpider | |
ECHA InfoCard | 100.000.149 |
KEGG | |
MeSH | Cortisone |
PubChem CID
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|
UNII | |
CompTox Dashboard (EPA)
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| |
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Properties | |
C21H28O5 | |
Molar mass | 360.450 g·mol−1 |
Melting point | 220 to 224 °C (428 to 435 °F; 493 to 497 K) |
Pharmacology | |
H02AB10 (WHO) S01BA03 (WHO) | |
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
|
Cortisone is a pregnene (21-carbon) steroid hormone. It is a naturally-occurring corticosteroid metabolite that is also used as a pharmaceutical prodrug. Cortisol is converted by the action of the enzyme corticosteroid 11-beta-dehydrogenase isozyme 2 into the inactive metabolite cortisone, particularly in the kidneys. This is done by oxidizing the alcohol group at carbon 11 (in the six-membered ring fused to the five-membered ring). Cortisone is converted back to the active steroid cortisol by stereospecific hydrogenation at carbon 11 by the enzyme 11β-Hydroxysteroid dehydrogenase type 1, particularly in the liver.
The term "cortisone" is frequently misused to mean either any corticosteroid or hydrocortisone, which is in fact cortisol. Many who speak of receiving a "cortisone shot" or taking "cortisone" are more likely receiving hydrocortisone or one of many other, much more potent synthetic corticosteroids.
Cortisone can be administered as a prodrug, meaning it has to be converted by the body (specifically the liver, converting it into cortisol) after administration to be effective. It is used to treat a variety of ailments and can be administered intravenously, orally, intra-articularly (into a joint), or transcutaneously. Cortisone suppresses various elements of the immune system, thus reducing inflammation and attendant pain and swelling. Risks exist, in particular in the long-term use of cortisone.[1][2] However, using cortisone only results in very mild activity, and very often more potent steroids are used instead.
Effects and uses
[edit]Cortisone itself is inactive.[3] It must be converted to cortisol by the action of 11β-hydroxysteroid dehydrogenase type 1.[4] This primarily happens in the liver, the main site at which cortisone becomes cortisol after oral or systemic injection, and can thus have a pharmacological effect. After application to the skin or injection into a joint, local cells that express 11β-hydroxysteroid dehydrogenase type 1 instead convert it to active cortisol.
A cortisone injection may provide short-term pain relief and may reduce the swelling from inflammation of a joint, tendon, or bursa in, for example, the joints of the knee, elbow and shoulder[1] and into a broken coccyx.[5]
Cortisone is used by dermatologists to treat keloids,[6] relieve the symptoms of eczema and atopic dermatitis,[7] and stop the development of sarcoidosis.[8]
Side effects
[edit]Oral use of cortisone has a number of potential systemic adverse effects, including asthma, hyperglycemia, insulin resistance, diabetes mellitus, osteoporosis, anxiety, depression, amenorrhoea, cataracts, glaucoma, Cushing's syndrome, increased risk of infections, and impaired growth.[1][2] With topical application, it can lead to thinning of the skin, impaired wound healing, increased skin pigmentation, tendon rupture, and skin infections (including abscesses).[9]
History
[edit]Cortisone was first identified by the American chemists Edward Calvin Kendall and Harold L. Mason while researching at the Mayo Clinic.[10][11][12] During the discovery process, cortisone was known as compound E (while cortisol was known as compound F).
In 1949, Philip S. Hench and colleagues discovered that large doses of injected cortisone were effective in the treatment of patients with severe rheumatoid arthritis.[13] Kendall was awarded the 1950 Nobel Prize for Physiology or Medicine along with Philip Showalter Hench and Tadeusz Reichstein for the discovery of the structure and function of adrenal cortex hormones including cortisone.[14][15] Both Reichstein and the team of O. Wintersteiner and J. Pfiffner had separately isolated the compound prior to the discovery made by Mason and Kendall, but failed to recognize its biological significance.[11] Mason's contributions to the crystallization and characterization of the compound have generally been forgotten outside of the Mayo Clinic.[11]
Cortisone was first produced commercially by Merck & Co. in 1948 or 1949.[13][16] On September 30, 1949, Percy Julian announced an improvement in the process of producing cortisone from bile acids.[17] This eliminated the need to use osmium tetroxide, a rare, expensive, and dangerous chemical. In the UK in the early 1950s, John Cornforth and Kenneth Callow at the National Institute for Medical Research collaborated with Glaxo to produce cortisone from hecogenin from sisal plants.[18]
Production
[edit]Cortisone is one of several end-products of a process called steroidogenesis. This process starts with the synthesis of cholesterol, which then proceeds through a series of modifications in the adrenal gland to become any one of many steroid hormones. One end-product of this pathway is cortisol. For cortisol to be released from the adrenal gland, a cascade of signaling occurs. Corticotropin-releasing hormone released from the hypothalamus stimulates corticotrophs in the anterior pituitary to release ACTH, which relays the signal to the adrenal cortex. Here, the zona fasciculata and zona reticularis, in response to ACTH, secrete glucocorticoids, in particular cortisol. In various peripheral tissues, notably the kidneys, cortisol is inactivated to cortisone by the enzyme corticosteroid 11-beta-dehydrogenase isozyme 2. This is crucial because cortisol is a potent mineralocorticoid and would cause havoc with electrolyte levels (raising blood sodium and lowering blood potassium levels) and raise blood pressure if it were not inactivated in the kidneys.[4]
Because cortisone must be converted to cortisol before being active as a glucocorticoid, its activity is less than simply administering cortisol directly (80–90%).[19]
Popular culture
[edit]Abuse and addiction to cortisone was the subject of the 1956 motion picture Bigger Than Life, produced by and starring James Mason. Though it was a box-office flop upon its initial release,[20] many modern critics hail the film as a masterpiece and brilliant indictment of contemporary attitudes toward mental illness and addiction.[21] In 1963, Jean-Luc Godard named it one of the ten greatest American sound films ever made.[22]
John F. Kennedy was regularly administered corticosteroids such as cortisone as a treatment for Addison's disease.[23]
See also
[edit]External links
[edit]- Media related to Cortisone at Wikimedia Commons
Notes
[edit]- ^ a b c "Cortisone shots". MayoClinic.com. 2010-11-16. Retrieved July 31, 2013.
- ^ a b "Prednisone and other corticosteroids: Balance the risks and benefits". MayoClinic.com. 2010-06-05. Retrieved 2017-12-21.
- ^ Martindale, William; Reynolds, James, eds. (1993). Martindale, The Extra Pharmacopoeia (30th ed.). Pharmaceutical Press. p. 726. ISBN 978-0853693000.
- ^ a b Cooper MS, Stewart PM (2009). "11Beta-hydroxysteroid dehydrogenase type 1 and its role in the hypothalamus-pituitary-adrenal axis, metabolic syndrome, and inflammation". J Clin Endocrinol Metab. 94 (12): 4645–4654. doi:10.1210/jc.2009-1412. PMID 19837912.
- ^ "injections and needles for coccyx pain". www.coccyx.org.
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