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Phenacetin

February 26, 2024

Phenacetin (acetophenetidin, N-(4-ethoxyphenyl)acetamide[1]) is a pain-relieving and fever-reducing drug, which was widely used following its introduction in 1887. It was withdrawn from medicinal use as dangerous from the 1970s (e.g., withdrawn in Canada in 1973,[2] and by the U.S. Food and Drug Administration in 1983[3]).

Phenacetin
Clinical data
ATC code
Identifiers
  • N-(4-Ethoxyphenyl)acetamide
CAS Number
  • 62-44-2 Y
PubChem CID
  • 4754
IUPHAR/BPS
  • 7402
DrugBank
  • DB03783 Y
ChemSpider
  • 4590 Y
UNII
  • ER0CTH01H9
KEGG
  • D00569 Y
ChEBI
  • CHEBI:8050 Y
ChEMBL
  • ChEMBL16073 Y
CompTox Dashboard (EPA)
  • DTXSID1021116
ECHA InfoCard100.000.485
Chemical and physical data
FormulaC10H13NO2
Molar mass179.219 g·mol−1
3D model (JSmol)
  • Interactive image
Density1.24 g/cm3
Melting point134 to 137.5 °C (273.2 to 279.5 °F)
Solubility in water0.766 g/L (25 °C (77 °F))
  • O=C(Nc1ccc(OCC)cc1)C
  • InChI=1S/C10H13NO2/c1-3-13-10-6-4-9(5-7-10)11-8(2)12/h4-7H,3H2,1-2H3,(H,11,12) Y
  • Key:CPJSUEIXXCENMM-UHFFFAOYSA-N Y
  (verify)

History edit

Phenacetin was introduced in 1887 in Elberfeld, Germany by German company Bayer, and was used principally as an analgesic; it was one of the first synthetic fever reducers to go on the market. It is also known historically to be one of the first non-opioid analgesics without anti-inflammatory properties. Although paracetamol (acetaminophen) was produced earlier, a historical accident saw it ignored after Joseph von Mering's 1893 assessment.[4]

Prior to World War One, Britain imported phenacetin from Germany.[5] During the war, a team including Jocelyn Field Thorpe and Martha Annie Whiteley developed a synthesis in Britain.[5]

Known mechanism of action edit

Phenacetin's analgesic effects are due to its actions on the sensory tracts of the spinal cord. In addition, phenacetin has a depressant action on the heart, where it acts as a negative inotrope. It is an antipyretic, acting on the brain to decrease the temperature set point. It is also used to treat rheumatoid arthritis (subacute type) and intercostal neuralgia.

In vivo, one of two reactions occur. Usually phenacetin's ether is cleaved to leave paracetamol (acetaminophen), which is the clinically relevant analgesic. A minority of the time the acetyl group is removed from the amine, producing carcinogenic p-phenetidine. This reaction is quite rare, however, as evidenced by the fact that the drug was on the market for almost 100 years before a statistical link was established, when Canada, followed by the United States, withdrew it from the market.

Preparation edit

The first synthesis was reported in 1878 by Harmon Northrop Morse. Morse's cited article describes the synthesis of paracetamol from 4-aminophenol and acetic acid.[6]

Phenacetin may be synthesized as an example of the Williamson ether synthesis: ethyl iodide, paracetamol, and anhydrous potassium carbonate are heated in 2-butanone to give the crude product, which is recrystallized from water.[7]

Uses edit

 
Vicks cold tablets, containing: salicylamide, phenacetin 2½ grs., pyrilamine maleate, caffeine, ephedrine sulphate, magnesium hydroxide, aluminum hydroxide complex (U.S. Pat. 2,446,981). That patent number is from 1948; these tablets would have been made shortly thereafter.

Medical edit

Phenacetin was widely used until the third quarter of the twentieth century, often in the form of an A.P.C., or "aspirin-phenacetin-caffeine" compound analgesic, as a remedy for fever and pain. An early formulation (1919) was Vincent's APC in Australia.

In the United States, the Food and Drug Administration ordered the withdrawal of drugs containing phenacetin in November 1983, due to its carcinogenic and kidney-damaging properties.[8] It was also banned in India.[9] As a result, some branded, and previously phenacetin-based, preparations continued to be sold, but with the phenacetin replaced by safer alternatives. A popular brand of phenacetin was Roche's Saridon, which was reformulated in 1983 to contain propyphenazone, paracetamol and caffeine. Coricidin was also reformulated without phenacetin. Paracetamol is a metabolite of phenacetin with similar analgesic and antipyretic effects, but the new formulation has not been found to have phenacetin's carcinogenicity.

Other edit

Phenacetin has been used as a cutting agent to adulterate cocaine in the UK and Canada, due to the similar physical properties.[10] There, it has been given the nickname "magic".

Due to its low cost, phenacetin is used for research into the physical and refractive properties of crystals. It is an ideal compound for this type of research.[why?][1][11]

In Canada, phenacetin is used as a laboratory reagent, and in a few hair dye preparations (as a stabilizer for hydrogen peroxide). While it is considered a prescription drug, no marketed drugs contain phenacetin.[12]

Safety edit

Phenacetin, and products containing phenacetin, have been shown in an animal model to have the side effect and after-effect of carcinogenesis. In humans, many case reports have implicated products containing phenacetin in urothelial neoplasms, especially urothelial carcinoma of the renal pelvis. Phenacetin is classified by the International Agency for Research on Cancer (IARC) as carcinogenic to humans.[1] In one prospective series, phenacetin was associated with an increased risk of death due to urologic or renal diseases, death due to cancers, and death due to cardiovascular diseases.[13] In addition, people with glucose-6-phosphate dehydrogenase deficiency may experience acute hemolysis, or dissolution of blood cells, while taking this drug. Acute hemolysis is possible in the case of patients who develop an IgM response to phenacetin leading to immune complexes that bind to erythrocytes in blood. The erythrocytes are then lysed when the complexes activate the complement system.

Chronic use of phenacetin is known to lead to analgesic nephropathy characterized by renal papillary necrosis.[14][15][16] This is a condition which results in destruction of some or all of the renal papillae in the kidneys. It is believed that the metabolite p-phenetidine is at least partly responsible for these effects.[17]

One notable death that can possibly be attributed to the use of this drug was that of the aviation pioneer Howard Hughes. He had been using phenacetin extensively for the treatment of chronic pain; it was stated during his autopsy that phenacetin use may have been the cause of his kidney failure.[18]

In popular culture edit

A 1974 episode of the Yorkshire Television series Justice, "Duty of Care", featured a court case that resulted from a woman dying of phenacetin poisoning, as a result of taking A.P.C. for five years. This explained that phenacetin caused renal papillary necrosis.[19]

In the book Zen and the Art of Motorcycle Maintenance chapter 4, "APCs for headaches" is included in a list of valuable things to take on motorcycle trips.[20]

See also edit

References edit

  1. ^ a b c Gralak B, Enoch S, Tayeb G (June 2000). "Anomalous refractive properties of photonic crystals". Journal of the Optical Society of America A. 17 (6): 1012–1020. Bibcode:2000JOSAA..17.1012G. CiteSeerX 10.1.1.462.8012. doi:10.1364/JOSAA.17.001012. PMID 10850471.
  2. ^ "Phenacetin". DrugBank. Retrieved 28 April 2020.
  3. ^ (PDF). Department of Health and Human Services - FDA. 5 October 1983. Archived from the original (PDF) on 30 September 2014.
  4. ^ Sneader W (2005). Drug Discovery: A History. Hoboken, NJ: Wiley. p. 439. ISBN 978-0471899808. from the original on 18 August 2016. The eminent clinical pharmacologist Joseph von Mering collaborated with the Bayer Company in a trial of paracetamol in 1893. He found it to be an effective antipyretic and analgesic, but claimed it had a slight tendency to produce methaemoglobinaemia. This could conceivably have been caused by the contamination of his paracetamol with the 4-aminophenol from which it was synthesised.
  5. ^ a b Creese MR (1997). "Martha Annie Whiteley (1866-1956): Chemist and Editor" (PDF). Bulletin for the History of Chemistry. 8: 42–45.
  6. ^ Morse HN (1878). "Ueber eine neue Darstellungsmethode der Acetylamidophenole". Berichte der deutschen chemischen Gesellschaft. 11 (1): 232–233. doi:10.1002/cber.18780110151.
  7. ^ . Chemistry Department Master Experiment Archive. California State University Stanislaus. Archived from the original on 2008-12-02.
  8. ^ Federal Register of October 5, 1983 (48 FR 45466)
  9. ^ . Central Drugs Standard Control Organization, Dte.GHS, Ministry of Health and Family Welfare, Government of India. Archived from the original on 2015-02-21. Retrieved 2013-09-17.
  10. ^ "Cancer chemical in street cocaine". BBC News. 23 November 2006.
  11. ^ Studenikin PA, Zagumennyi AI, Zavartsev YD, Popov PA, Shcherbakov IA (1995). "GdVO4as a new medium for solid-state lasers: Some optical and thermal properties of crystals doped with Cd3+, Tm3+, and Er3+ions". Quantum Electronics. 25 (12): 1162–1165. doi:10.1070/QE1995v025n12ABEH000556. S2CID 250787020.
  12. ^ "Health - Product safety - Chemical substances - Phenacetin information sheet". Government of Canada -. 18 April 2017. Retrieved 29 April 2020.
  13. ^ Dubach UC, Rosner B, Stürmer T (January 1991). "An epidemiologic study of abuse of analgesic drugs. Effects of phenacetin and salicylate on mortality and cardiovascular morbidity (1968 to 1987)". The New England Journal of Medicine. 324 (3): 155–160. doi:10.1056/NEJM199101173240304. PMID 1984193.
  14. ^ Cochran AJ, Lawson DH, Linton AL (July 1967). "Renal papillary necrosis following phenacetin excess". Scottish Medical Journal. 12 (7): 246–250. doi:10.1177/003693306701200702. PMID 6036245. S2CID 33774826.
  15. ^ Tan GH, Rabbino MD, Hopper J (August 1964). "Is Phenacetin a Nephrotoxin?: A Report on Twenty-three Users of the Drug". California Medicine. 101 (2): 73–77. PMC 1515485. PMID 14180501.
  16. ^ Brix AE (2002). "Renal papillary necrosis". Toxicologic Pathology. 30 (6): 672–674. doi:10.1080/01926230290166760. PMID 12512867.
  17. ^ Kankuri E, Solatunturi E, Vapaatalo H (June 2003). "Effects of phenacetin and its metabolite p-phenetidine on COX-1 and COX-2 activities and expression in vitro". Thrombosis Research. 110 (5–6): 299–303. doi:10.1016/S0049-3848(03)00416-X. PMID 14592552.
  18. ^ Tennant F (July–August 2007). (PDF). Practical Pain Management. 7 (6): 20. Archived from the original (PDF) on 24 September 2015. Retrieved 2 November 2015. The phenacetin in the codeine compound produced, over time, kidney failure and death.
  19. ^ "Duty of Care", Justice (1971 TV series), Yorkshire Television, 31 May 1974
  20. ^ Pirsig, Robert M. (1985). Zen and the Art of Motorcycle Maintenance (82nd printing ed.). Bantam. p. 35.

External links edit

 
Look up phenacetin in Wiktionary, the free dictionary.
  • IARC report
  • Safety (MSDS) data for phenacetin 2006-09-24 at the Wayback Machine

February 26, 2024
phenacetin, acetophenetidin, ethoxyphenyl, acetamide, pain, relieving, fever, reducing, drug, which, widely, used, following, introduction, 1887, withdrawn, from, medicinal, dangerous, from, 1970s, withdrawn, canada, 1973, food, drug, administration, 1983, cli. Phenacetin acetophenetidin N 4 ethoxyphenyl acetamide 1 is a pain relieving and fever reducing drug which was widely used following its introduction in 1887 It was withdrawn from medicinal use as dangerous from the 1970s e g withdrawn in Canada in 1973 2 and by the U S Food and Drug Administration in 1983 3 PhenacetinClinical dataATC codeN02BE03 WHO IdentifiersIUPAC name N 4 Ethoxyphenyl acetamideCAS Number62 44 2 YPubChem CID4754IUPHAR BPS7402DrugBankDB03783 YChemSpider4590 YUNIIER0CTH01H9KEGGD00569 YChEBICHEBI 8050 YChEMBLChEMBL16073 YCompTox Dashboard EPA DTXSID1021116ECHA InfoCard100 000 485Chemical and physical dataFormulaC 10H 13N O 2Molar mass179 219 g mol 13D model JSmol Interactive imageDensity1 24 g cm3Melting point134 to 137 5 C 273 2 to 279 5 F Solubility in water0 766 g L 25 C 77 F SMILES O C Nc1ccc OCC cc1 CInChI InChI 1S C10H13NO2 c1 3 13 10 6 4 9 5 7 10 11 8 2 12 h4 7H 3H2 1 2H3 H 11 12 YKey CPJSUEIXXCENMM UHFFFAOYSA N Y verify Contents 1 History 2 Known mechanism of action 3 Preparation 4 Uses 4 1 Medical 4 2 Other 5 Safety 6 In popular culture 7 See also 8 References 9 External linksHistory editPhenacetin was introduced in 1887 in Elberfeld Germany by German company Bayer and was used principally as an analgesic it was one of the first synthetic fever reducers to go on the market It is also known historically to be one of the first non opioid analgesics without anti inflammatory properties Although paracetamol acetaminophen was produced earlier a historical accident saw it ignored after Joseph von Mering s 1893 assessment 4 Prior to World War One Britain imported phenacetin from Germany 5 During the war a team including Jocelyn Field Thorpe and Martha Annie Whiteley developed a synthesis in Britain 5 Known mechanism of action editPhenacetin s analgesic effects are due to its actions on the sensory tracts of the spinal cord In addition phenacetin has a depressant action on the heart where it acts as a negative inotrope It is an antipyretic acting on the brain to decrease the temperature set point It is also used to treat rheumatoid arthritis subacute type and intercostal neuralgia In vivo one of two reactions occur Usually phenacetin s ether is cleaved to leave paracetamol acetaminophen which is the clinically relevant analgesic A minority of the time the acetyl group is removed from the amine producing carcinogenic p phenetidine This reaction is quite rare however as evidenced by the fact that the drug was on the market for almost 100 years before a statistical link was established when Canada followed by the United States withdrew it from the market Preparation editThe first synthesis was reported in 1878 by Harmon Northrop Morse Morse s cited article describes the synthesis of paracetamol from 4 aminophenol and acetic acid 6 Phenacetin may be synthesized as an example of the Williamson ether synthesis ethyl iodide paracetamol and anhydrous potassium carbonate are heated in 2 butanone to give the crude product which is recrystallized from water 7 Uses edit nbsp Vicks cold tablets containing salicylamide phenacetin 2 grs pyrilamine maleate caffeine ephedrine sulphate magnesium hydroxide aluminum hydroxide complex U S Pat 2 446 981 That patent number is from 1948 these tablets would have been made shortly thereafter Medical edit Phenacetin was widely used until the third quarter of the twentieth century often in the form of an A P C or aspirin phenacetin caffeine compound analgesic as a remedy for fever and pain An early formulation 1919 was Vincent s APC in Australia In the United States the Food and Drug Administration ordered the withdrawal of drugs containing phenacetin in November 1983 due to its carcinogenic and kidney damaging properties 8 It was also banned in India 9 As a result some branded and previously phenacetin based preparations continued to be sold but with the phenacetin replaced by safer alternatives A popular brand of phenacetin was Roche s Saridon which was reformulated in 1983 to contain propyphenazone paracetamol and caffeine Coricidin was also reformulated without phenacetin Paracetamol is a metabolite of phenacetin with similar analgesic and antipyretic effects but the new formulation has not been found to have phenacetin s carcinogenicity Other edit Phenacetin has been used as a cutting agent to adulterate cocaine in the UK and Canada due to the similar physical properties 10 There it has been given the nickname magic Due to its low cost phenacetin is used for research into the physical and refractive properties of crystals It is an ideal compound for this type of research why 1 11 In Canada phenacetin is used as a laboratory reagent and in a few hair dye preparations as a stabilizer for hydrogen peroxide While it is considered a prescription drug no marketed drugs contain phenacetin 12 Safety editPhenacetin and products containing phenacetin have been shown in an animal model to have the side effect and after effect of carcinogenesis In humans many case reports have implicated products containing phenacetin in urothelial neoplasms especially urothelial carcinoma of the renal pelvis Phenacetin is classified by the International Agency for Research on Cancer IARC as carcinogenic to humans 1 In one prospective series phenacetin was associated with an increased risk of death due to urologic or renal diseases death due to cancers and death due to cardiovascular diseases 13 In addition people with glucose 6 phosphate dehydrogenase deficiency may experience acute hemolysis or dissolution of blood cells while taking this drug Acute hemolysis is possible in the case of patients who develop an IgM response to phenacetin leading to immune complexes that bind to erythrocytes in blood The erythrocytes are then lysed when the complexes activate the complement system Chronic use of phenacetin is known to lead to analgesic nephropathy characterized by renal papillary necrosis 14 15 16 This is a condition which results in destruction of some or all of the renal papillae in the kidneys It is believed that the metabolite p phenetidine is at least partly responsible for these effects 17 One notable death that can possibly be attributed to the use of this drug was that of the aviation pioneer Howard Hughes He had been using phenacetin extensively for the treatment of chronic pain it was stated during his autopsy that phenacetin use may have been the cause of his kidney failure 18 In popular culture editA 1974 episode of the Yorkshire Television series Justice Duty of Care featured a court case that resulted from a woman dying of phenacetin poisoning as a result of taking A P C for five years This explained that phenacetin caused renal papillary necrosis 19 In the book Zen and the Art of Motorcycle Maintenance chapter 4 APCs for headaches is included in a list of valuable things to take on motorcycle trips 20 See also editBucetinReferences edit a b c Gralak B Enoch S Tayeb G June 2000 Anomalous refractive properties of photonic crystals Journal of the Optical Society of America A 17 6 1012 1020 Bibcode 2000JOSAA 17 1012G CiteSeerX 10 1 1 462 8012 doi 10 1364 JOSAA 17 001012 PMID 10850471 Phenacetin DrugBank Retrieved 28 April 2020 Drugs withdrawn from the market containing phenacetin PDF Department of Health and Human Services FDA 5 October 1983 Archived from the original PDF on 30 September 2014 Sneader W 2005 Drug Discovery A History Hoboken NJ Wiley p 439 ISBN 978 0471899808 Archived from the original on 18 August 2016 The eminent clinical pharmacologist Joseph von Mering collaborated with the Bayer Company in a trial of paracetamol in 1893 He found it to be an effective antipyretic and analgesic but claimed it had a slight tendency to produce methaemoglobinaemia This could conceivably have been caused by the contamination of his paracetamol with the 4 aminophenol from which it was synthesised a b Creese MR 1997 Martha Annie Whiteley 1866 1956 Chemist and Editor PDF Bulletin for the History of Chemistry 8 42 45 Morse HN 1878 Ueber eine neue Darstellungsmethode der Acetylamidophenole Berichte der deutschen chemischen Gesellschaft 11 1 232 233 doi 10 1002 cber 18780110151 Conversion of Acetaminophen into Phenacetin Chemistry Department Master Experiment Archive California State University Stanislaus Archived from the original on 2008 12 02 Federal Register of October 5 1983 48 FR 45466 Drugs banned in India Central Drugs Standard Control Organization Dte GHS Ministry of Health and Family Welfare Government of India Archived from the original on 2015 02 21 Retrieved 2013 09 17 Cancer chemical in street cocaine BBC News 23 November 2006 Studenikin PA Zagumennyi AI Zavartsev YD Popov PA Shcherbakov IA 1995 GdVO4as a new medium for solid state lasers Some optical and thermal properties of crystals doped with Cd3 Tm3 and Er3 ions Quantum Electronics 25 12 1162 1165 doi 10 1070 QE1995v025n12ABEH000556 S2CID 250787020 Health Product safety Chemical substances Phenacetin information sheet Government of Canada 18 April 2017 Retrieved 29 April 2020 Dubach UC Rosner B Sturmer T January 1991 An epidemiologic study of abuse of analgesic drugs Effects of phenacetin and salicylate on mortality and cardiovascular morbidity 1968 to 1987 The New England Journal of Medicine 324 3 155 160 doi 10 1056 NEJM199101173240304 PMID 1984193 Cochran AJ Lawson DH Linton AL July 1967 Renal papillary necrosis following phenacetin excess Scottish Medical Journal 12 7 246 250 doi 10 1177 003693306701200702 PMID 6036245 S2CID 33774826 Tan GH Rabbino MD Hopper J August 1964 Is Phenacetin a Nephrotoxin A Report on Twenty three Users of the Drug California Medicine 101 2 73 77 PMC 1515485 PMID 14180501 Brix AE 2002 Renal papillary necrosis Toxicologic Pathology 30 6 672 674 doi 10 1080 01926230290166760 PMID 12512867 Kankuri E Solatunturi E Vapaatalo H June 2003 Effects of phenacetin and its metabolite p phenetidine on COX 1 and COX 2 activities and expression in vitro Thrombosis Research 110 5 6 299 303 doi 10 1016 S0049 3848 03 00416 X PMID 14592552 Tennant F July August 2007 Howard Hughes amp Pseudoaddiction PDF Practical Pain Management 7 6 20 Archived from the original PDF on 24 September 2015 Retrieved 2 November 2015 The phenacetin in the codeine compound produced over time kidney failure and death Duty of Care Justice 1971 TV series Yorkshire Television 31 May 1974 Pirsig Robert M 1985 Zen and the Art of Motorcycle Maintenance 82nd printing ed Bantam p 35 External links edit nbsp Look up phenacetin in Wiktionary the free dictionary Carcinogen report from the NIH IARC report Safety MSDS data for phenacetin Archived 2006 09 24 at the Wayback Machine Retrieved from https en wikipedia org w index php title Phenacetin amp oldid 1195990285, wikipedia, wiki, book, books, library,

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