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Benoxaprofen
Clinical data
ATC code	M01AE06 (WHO) ;
Identifiers
	IUPAC name 2-[2-(4-chlorophenyl)-1,3-benzoxazol-5-yl]propanoic acid;
CAS Number	51234-28-7 ;
PubChem CID	39941;
DrugBank	DB04812 ;
ChemSpider	36518 ;
UNII	17SZX404IM;
ChEBI	CHEBI:76114 ;
ChEMBL	ChEMBL340978 ;
E number	{{#property:P628}}
ECHA InfoCard	{{#property:P2566}}Lua error in Module:EditAtWikidata at line 36: attempt to index field 'wikibase' (a nil value).
Chemical and physical data
Formula	C16H12ClNO3
Molar mass	301.72438 g/mol
3D model (JSmol)	Interactive image;
	SMILES O=C(O)C(c1cc2nc(oc2cc1)c3ccc(Cl)cc3)C;
	InChI InChI=1S/C16H12ClNO3/c1-9(16(19)20)11-4-7-14-13(8-11)18-15(21-14)10-2-5-12(17)6-3-10/h2-9H,1H3,(H,19,20) ; Key:MITFXPHMIHQXPI-UHFFFAOYSA-N ;
(what is this?) (verify)

VisualWikitext

Latest revision as of 17:59, 18 August 2015

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]

Overview

Benoxaprofen is a chemical compound with the formula C₁₆H₁₂ClNO₃. It is a non-steroidal anti-inflammatory drug and was marketed under the brand name Oraflex in the United States and as Opren in Europe by Eli Lilly and Company. Lilly suspended sales of Oraflex in 1982 after reports from the British government and the U.S. Food and Drug Administration (FDA) of adverse effects and deaths linked to the drug.

History

Benoxaprofen was discovered by a team of Lilly chemists at its British laboratory. This laboratory was assigned to explore new anti-arthritic compounds in 1966. Lilly applied for patents on benoxaprofen seven years later and also filed for permission from the FDA to start testing the drug on humans. It had to undergo the three-step clinical testing procedure required by the Federal Government.

Lilly began Phase I of the progress by testing a handful of healthy human volunteers. These tests had to prove that the drug posed no clear and immediate safety hazards. In Phase II a larger number of human subjects, including some with minor illnesses, was tested. The drug’s effectiveness and safety was the major target of these tests. Phase III was the largest test and began in 1976. More than 2,000 arthritis patients were administered the drug by more than 100 physicians. The physicians reported the results to the Lilly Company.

When the company formally requested to begin marketing the drug in January 1980 with the FDA, the document consisted of more than 100,000 pages of test results and patients’ records. Benoxaprofen was first marketed abroad: in 1980 the drug was released for marketing in the UK. It came on the market in May 1982 in the USA.

When benoxaprofen was on the market as Oraflex in the USA the first sign of trouble came for the Lilly Company. The British Medical Journal reported in May 1982 that physicians in the UK believed that the drug was responsible for at least 12 deaths, mainly caused by kidney and liver failure. A petition was filed to have Oraflex removed from the market.

On the fourth of August 1982 the British government temporarily suspended sales of the drug in UK ‘on grounds of safety’. The British Committee on the Safety of Medicines declared, in a telegram to the FDA, that it had received reports of more than 3,500 adverse side-effects among patients who had used Oraflex. There were also 61 deaths, most of which were of elderly people. Almost simultaneously, the FDA said it had reports of 11 deaths in the USA among Oraflex users, most of which were caused by kidney and liver damage. The Eli Lilly Company suspended sales of benoxaprofen that afternoon.

Structure and reactivity

The molecular formula of benoxaprofen is C₁₆H₁₂ClNO₃ and the systematic (IUPAC) name is 2-[2-(4-chlorophenyl)-1,3-benzoxazol-5-yl]propionic acid. The molecule has a molecular mass of 301.050568 g/mol. Benoxaprofen is essentially a planar molecule. This is due to the co-planarity of the benzoxazole and phenyl rings, but the molecule also has a non-planar side chain consisting of the propanoic acid moiety which acts as a carrier group. These findings were determined with the use of X-ray crystallographic measurements by the Lilly Research Centre Limited.

Furthermore, benoxaprofen is highly phototoxic. The free radical decarboxylated derivative of the drug is the toxic agent which, in the presence of oxygen, yields singlet oxygen and superoxy anion. Photochemical decarboxylation via a radical mechanism and in single-strand breaks of DNA is caused by irradiation of benoxaprofen in an aqueous solution. This also happens to ketoprofen and naproxen, other non-steroidal anti-inflammatory drugs, which are even more active in this respect than benoxaprofen.

Available forms

Benoxaprofen is a racemic mixture [(RS)-2-(p-chlorophenyl-a-methyl-5-benzoxazoleacetic acid]. The two enantiomers are R(-) and S(+).

The inversion of the R(-) enantiomer and glucuronide conjugation will metabolize benoxaprofen. However, benoxaprofen will not readily undergo oxidative metabolism.

It is however possible that, when cytochrome P4501 is the catalyst, oxygenation of the 4-chlorophyl ring occurs. With the S(+) enantiomer it is more likely that oxygenation of the aromatic ring of the 2-phenylpropionic acid moiety occurs, also here is cytochrome P4501 the catalyst.

Toxicokinetics

Benoxaprofen is absorbed well after oral intake of doses ranging from 1 up to 10 mg/kg. Only the unchanged drug is detected in the plasma, mostly bound to plasma proteins.[6] The plasma levels of benoxaprofen in eleven subjects have been accurately predicted, based on the two-compartment open model. The mean half-life of absorption was 0.4 hours. This means that within 25 minutes, half of the dose is absorbed in the system. The mean half-life of distribution was 4.8 hours. This means that within 5 hours, half of the dose is distributed throughout the entire system. The mean half-life of elimination was 37.8 hours. This means that within 40 hours, half of the dose is excreted out of the system.

In female rats, after oral dose of 20 mg/kg, the tissue concentration of benoxaprofen was the highest in liver, kidney, lungs, adrenals and ovaries. The distribution in pregnant females is the same, while it can also be found –in lower concentrations– in the foetus. There is a big difference between species in the route of excretion. In man, rhesus monkey and rabbit it is mostly excreted via the urine, while in rat and dog is was excreted via biliary-faecal excretion. In man and dog, the compound was excreted as the ester glucuronide, and in the other species as the unchanged compound. This means no major metabolic transformation of benoxaprofen takes place.

Toxicodynamics

Unlike other non-steroidal anti-inflammatory compounds, benoxaprofen acts directly on mononuclear cells. It inhibits their chemotactic response by inhibiting the lipoxygenase enzyme.

Efficacy and side effects

Efficacy

Benoxaprofen is an analgesic, antipyretic and anti-inflammatory drug. Benoxaprofen was given to patients with rheumatoid arthritis and osteoarthritis because of its anti-inflammatory effect. Patients with the Paget’s disease, psoriatic arthritis, ankylosing spondylitis, a painful shoulder, the mixed connective-tissue disease, polymyalgia rheumatica, back pain and the Behçet’s disease received benoxaprofen, too. A daily dose of 300–600 mg is effective for many patients.

Adverse effects

There are different types of side effects. Most of them were cutaneous or gastrointestinal. Side effects appear rarely in the central nervous system and miscellaneous side effects were not often observed. A study shows that most side effects appear in patients with rheumatoid arthritis

Cutaneous side effects

Cutaneous side effects of benoxaprofen are photosensitivity, onycholysis, rash, milia, increased nail growth, pruritus (itch) and hypertrichosis. Photosensitivity leads to burning, itching or redness when patients are exposed to sunlight. A study shows that benoxaprofen, or other lipoxygenase-inhibiting agents, might be helpful in the treatment of psoriasis because the migration inhibition of the inflammatory cells (leukocytes) into the skin.

Gastrointestinal side effects

Gastrointestinal side effects of benoxaprofen are bleeding, diarrhoea, abdominal pain, anorexia (symptom), mouth ulcers and taste change. According to a study the most appearing gastric side effects are vomiting, heartburn and epigastric pain.

Side effects in the central nervous system

For a small number of people, taking benoxaprofen might result in depression, lethargy and feeling ill.

Miscellaneous side effects

Faintness, dizziness, headache, palpitations, epistaxis, blurred vision, urinary urgency and gynaecomastia rarely appear in patients who take benoxaprofen. Benoxaprofen also causes hepatotoxicity, which led to death of some elderly patients. That was the main reason why the drug was withdrawn from the market.

Toxicity

After the suspension of sales in 1982 the toxic effects which benoxaprofen might have on humans were looked into more deeply. The fairly planar compound of benoxaprofen seems to be hepa- and phototoxic in the human body.

Benoxaprofen has a rather long half life in man (t_1/2= 20-30 h), undergoes biliary excretion and enterohepatic circulation and is also known to have a slow plasma clearance (CL p=4.5 ml/min). The half life may be further increased in elderly patients (>80 years of age) and in patients which already have an renal impairment increasing to figures as high as 148 hours.

The fetal hepatotoxicity of benoxaprofen can be attributed to the accumulation of the drug after a repeated dosage and also associated with the slow plasma clearance. The hepatic accumulation of the drug is presumably the cause for an increase in the activity of the hepatic cytochrome P450I which will oxygenate benaxoprofen and produce reactive intermediates. Benoxaprofen is very likely a substrate and weak inducer of cytochrome P450I and its enzyme family. Normally it is not metabolized by oxidative reactions but with the S(+) enantiomer of benoxaprofen and cytochrome P450I as a catalyst the oxygenation of the 4-chlorophenyl ring and of the aromatic ring of 2-phenyl propionic acid seems to be possible. Therefore the induction of a minor metabolic pathway leads to the formation of toxic metabolites in considerable amounts. The toxic metabolites may bind to vital intracellular macromolecules and may generate reactive oxygens by redox cycling if quinone is formed. This could also lead to a depletion of protective glutathione which is responsible for the detoxification of reactive oxygens.

The observed skin phototoxicity of patients treated with benoxaprofen can be explained with a look at the structure of the compound. There are significant structural similarities between the benzoxazole ring of benoxaprofen and the benzafuran ring of psoralen, a compound known to be phototoxic. The free decarboxylated derivate of the drug can produce singlet oxygen and superoxy anions in the presence of oxygen. Furthermore possible explanations for the photochemical decarboxylation and oxygen radical formation may be the accumulation of repeated dosage, the induction of cytochrome P450I and the emergence of reactive intermediates with covalent binding. The photochemical character of the compound can cause inflammation and severe tissue damage.

In animals peroxisomal proliferation is also observed but does not seem to be significant in man.

Effects on animals

The effects of Benoxaprofen on animals were tested in a series of experiments. Benoxaprofen had a considerably anti-inflammatory, analgesic and also anti-pyretic activity in those tests. In all six animals tested, which included rats, dogs, rhesus monkeys, rabbits, guinea pigs and mice, the drug was well absorbed orally. In three of the six species benoxaprofen was then effectively taken up from the gastrointestinal tract (after oral doses of 1–10 mg/kg). The plasma half life was found to be different, being less than 13 hours in the dog, rabbit and monkey, it was notable longer in mice. Furthermore there were species differences found in the rate and route of excretion of the compound. Whereas benoxaprofen was excreted into the urine by the rabbit and guinea pig, biliary excretion was the way of clearance found in rats and dogs. In all species only unchanged benoxaprofen was found in the plasma mostly extensively bound to proteins.

The excretion of the unchanged compound into the bile did occur more slowly in rats. This is interpreted by the authors as evidence that no enterohepatic circulation takes place. Another research in rats showed that the plasma membrane of hepatocytes begun to form blebs after administration of benoxaprofen. This is suggested to be due to disturbances in the calcium concentration which is possibly a result of an altered cellular redox state which can have an effect on mitochondrial function and therefore cause disturbances in the calcium concentration. In none of the species significant levels of metabolism of benoxaprofen were found to have happened. Only in dogs glucuronide could be found in the bile which is a sure sign of metabolism in that species. Also no differences in distribution of the compound in normal and pregnant rats were found. It was shown in rats that benoxaprofen was distributed into the foetus but with a notable lower concentration than in the maternal tissue.

References

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 {{CMG}}
 ==Overview==
 '''Benoxaprofen''' is a chemical compound with the formula C<sub>16</sub>H<sub>12</sub>ClNO<sub>3</sub>. It is a [[non-steroidal anti-inflammatory drug]] and was marketed under the brand name '''Oraflex''' in the United States and as '''Opren''' in Europe by [[Eli Lilly and Company]]. Lilly suspended sales of Oraflex in 1982 after reports from the British government and the U.S. [[Food and Drug Administration]] (FDA) of adverse effects and deaths linked to the drug.
 ==History==
-Benoxaprofen was discovered by a team of Lilly chemists at its British laboratory. This laboratory was assigned to explore new anti-arthritic compounds in 1966. Lilly applied for patents on benoxaprofen seven years later and also filed for permission from the FDA to start testing the drug on humans. It had to undergo the three-step clinical testing procedure required by the Federal Government.<ref name="At Lilly">[http://query.nytimes.com/gst/fullpage.html?sec=health&res=9804E7D91E39F936A2575BC0A964948260 New York Times - At Lilly, the Side-Effects Of Oraflex]</ref>
+Benoxaprofen was discovered by a team of Lilly chemists at its British laboratory. This laboratory was assigned to explore new anti-arthritic compounds in 1966. Lilly applied for patents on benoxaprofen seven years later and also filed for permission from the FDA to start testing the drug on humans. It had to undergo the three-step clinical testing procedure required by the Federal Government.
-Lilly began Phase I of the progress by testing a handful of healthy human volunteers. These tests had to prove that the drug posed no clear and immediate safety hazards. In Phase II a larger number of human subjects, including some with minor illnesses, was tested. The drug’s effectiveness and safety was the major target of these tests. Phase III was the largest test and began in 1976. More than 2,000 arthritis patients were administered the drug by more than 100 physicians. The physicians reported the results to the Lilly Company.<ref name="At Lilly" />
+Lilly began Phase I of the progress by testing a handful of healthy human volunteers. These tests had to prove that the drug posed no clear and immediate safety hazards. In Phase II a larger number of human subjects, including some with minor illnesses, was tested. The drug’s effectiveness and safety was the major target of these tests. Phase III was the largest test and began in 1976. More than 2,000 arthritis patients were administered the drug by more than 100 physicians. The physicians reported the results to the Lilly Company.
 When the company formally requested to begin marketing the drug in January 1980 with the FDA, the document consisted of more than 100,000 pages of test results and patients’ records.
-Benoxaprofen was first marketed abroad: in 1980 the drug was released for marketing in the UK. It came on the market in May 1982 in the USA.<ref>G., R.; The rise and fall of Benoxaprofen. Rheumatology and Rehabilitation; November 1982, Vol. XXI, No. 4</ref>
+Benoxaprofen was first marketed abroad: in 1980 the drug was released for marketing in the UK. It came on the market in May 1982 in the USA.
-When benoxaprofen was on the market as Oraflex in the USA the first sign of trouble came for the Lilly Company. The British Medical Journal reported in May 1982 that physicians in the UK believed that the drug was responsible for at least 12 deaths, mainly caused by kidney and liver failure. A petition was filed to have Oraflex removed from the market.<ref name="At Lilly" />
+When benoxaprofen was on the market as Oraflex in the USA the first sign of trouble came for the Lilly Company. The British Medical Journal reported in May 1982 that physicians in the UK believed that the drug was responsible for at least 12 deaths, mainly caused by kidney and liver failure. A petition was filed to have Oraflex removed from the market.
-On the fourth of August 1982 the British government temporarily suspended sales of the drug in UK ‘on grounds of safety’. The British Committee on the Safety of Medicines declared, in a telegram to the FDA, that it had received reports of more than 3,500 adverse side-effects among patients who had used Oraflex. There were also 61 deaths, most of which were of elderly people. Almost simultaneously, the FDA said it had reports of 11 deaths in the USA among Oraflex users, most of which were caused by kidney and liver damage.<ref name="At Lilly" />
+On the fourth of August 1982 the British government temporarily suspended sales of the drug in UK ‘on grounds of safety’. The British Committee on the Safety of Medicines declared, in a telegram to the FDA, that it had received reports of more than 3,500 adverse side-effects among patients who had used Oraflex. There were also 61 deaths, most of which were of elderly people. Almost simultaneously, the FDA said it had reports of 11 deaths in the USA among Oraflex users, most of which were caused by kidney and liver damage.
+The Eli Lilly Company suspended sales of benoxaprofen that afternoon.
-The Eli Lilly Company suspended sales of benoxaprofen that afternoon.<ref name="At Lilly" />
 ==Structure and reactivity==
-The molecular formula of benoxaprofen is C<sub>16</sub>H<sub>12</sub>ClNO<sub>3</sub> and the systematic (IUPAC) name is 2-[2-(4-chlorophenyl)-1,3-benzoxazol-5-yl]propionic acid. The molecule has a molecular mass of 301.050568 g/mol.<ref>[http://www.chemspider.com/Chemical-Structure.36518.html ChemSpider Benoxaprofen]</ref>
+The molecular formula of benoxaprofen is C<sub>16</sub>H<sub>12</sub>ClNO<sub>3</sub> and the systematic (IUPAC) name is 2-[2-(4-chlorophenyl)-1,3-benzoxazol-5-yl]propionic acid. The molecule has a molecular mass of 301.050568 g/mol.
+Benoxaprofen is essentially a planar molecule. This is due to the co-planarity of the benzoxazole and phenyl rings, but the molecule also has a non-planar side chain consisting of the propanoic acid moiety which acts as a carrier group. These findings were determined with the use of  X-ray crystallographic measurements by the Lilly Research Centre Limited.
-Benoxaprofen is essentially a planar molecule. This is due to the co-planarity of the benzoxazole and phenyl rings, but the molecule also has a non-planar side chain consisting of the propanoic acid moiety which acts as a carrier group. These findings were determined with the use of  X-ray crystallographic measurements by the Lilly Research Centre Limited.<ref name="Lewis">D.F.V. Lewis, C. Ioannides and D.V. Parker; A retrospective study of the molecular toxicology of benoxaprofen. Department of Biochemistry, University of Surrey, Guildford, Surrey, Toxicology, 65 (1990) 33—47, Elsevier Scientific Publishers Ireland Ltd.</ref>
 Furthermore, benoxaprofen is highly phototoxic. The free radical decarboxylated derivative of the drug is the toxic agent which, in the presence of oxygen, yields singlet oxygen and superoxy anion.
-Photochemical decarboxylation via a radical mechanism and in single-strand breaks of DNA is caused by irradiation of benoxaprofen in an aqueous solution. This also happens to ketoprofen and naproxen, other non-steroidal anti-inflammatory drugs, which are even more active in this respect than benoxaprofen.<ref name="Lewis"/>
+Photochemical decarboxylation via a radical mechanism and in single-strand breaks of DNA is caused by irradiation of benoxaprofen in an aqueous solution. This also happens to ketoprofen and naproxen, other non-steroidal anti-inflammatory drugs, which are even more active in this respect than benoxaprofen.
 ==Available forms==
-Benoxaprofen is a [[racemic mixture]] [(RS)-2-(p-chlorophenyl-a-methyl-5-benzoxazoleacetic acid]. The two [[enantiomers]] are R(-) and S(+).<ref name="Bopp">5.	R.J. Bopp, J.F. Nash, A.S. Ridolfo, and E.R. Shepard; Stereoselective inversion of (R)-(−)-benoxaprofen to the (S)-(+)-enantiomer in humans. Department of Analytical Development, Lilly Research Laboratories, Drug Metabolism and Disposition, 1979, Vol. 7, No. 6</ref>
+Benoxaprofen is a [[racemic mixture]] [(RS)-2-(p-chlorophenyl-a-methyl-5-benzoxazoleacetic acid]. The two [[enantiomers]] are R(-) and S(+).
-The inversion of the R(-) enantiomer and [[glucuronide]] conjugation will metabolize benoxaprofen. However, benoxaprofen will not readily undergo oxidative metabolism.<ref name="Lewis"/>
+The inversion of the R(-) enantiomer and [[glucuronide]] conjugation will metabolize benoxaprofen. However, benoxaprofen will not readily undergo oxidative metabolism.
-It is however possible that, when [[Cytochrome P450#CYP families in humans|cytochrome P4501]] is the catalyst, oxygenation of the 4-chlorophyl ring occurs. With the S(+) enantiomer it is more likely that oxygenation of the aromatic ring of the 2-phenylpropionic acid moiety occurs, also here is cytochrome P4501 the catalyst.<ref name="Lewis"/>
+It is however possible that, when [[Cytochrome P450#CYP families in humans|cytochrome P4501]] is the catalyst, oxygenation of the 4-chlorophyl ring occurs. With the S(+) enantiomer it is more likely that oxygenation of the aromatic ring of the 2-phenylpropionic acid moiety occurs, also here is cytochrome P4501 the catalyst.
 ==Toxicokinetics==
-Benoxaprofen is absorbed well after oral intake of doses ranging from 1 up to 10&nbsp;mg/kg. Only the unchanged drug is detected in the plasma, mostly bound to plasma proteins.[6] The plasma levels of benoxaprofen  in eleven subjects have been accurately predicted, based on the two-compartment open model. The mean half-life of absorption was 0.4 hours. This means that within 25 minutes, half of the dose is absorbed in the system. The mean half-life of distribution was 4.8 hours. This means that within 5 hours, half of the dose is distributed throughout the entire system. The mean half-life of elimination was 37.8 hours. This means that within 40 hours, half of the dose is excreted out of the system.<ref>D.H. Chatfield, M.E. Tarrant, G.L. Smith, C.F. Speirs; Pharmacokinetic studies with benoxaprofen in man: prediction of steady-state levels from single-dose data. Lilly Research Centre Ltd, Erl Wood Manor, Windlesham, Surrey GU20 6PH Br. J. clin. Pharmac. (1977), 4, 579-583</ref>
+Benoxaprofen is absorbed well after oral intake of doses ranging from 1 up to 10&nbsp;mg/kg. Only the unchanged drug is detected in the plasma, mostly bound to plasma proteins.[6] The plasma levels of benoxaprofen  in eleven subjects have been accurately predicted, based on the two-compartment open model. The mean half-life of absorption was 0.4 hours. This means that within 25 minutes, half of the dose is absorbed in the system. The mean half-life of distribution was 4.8 hours. This means that within 5 hours, half of the dose is distributed throughout the entire system. The mean half-life of elimination was 37.8 hours. This means that within 40 hours, half of the dose is excreted out of the system.
-In female rats, after oral dose of 20&nbsp;mg/kg, the tissue concentration of benoxaprofen was the highest in liver, kidney, lungs, adrenals and ovaries. The distribution in pregnant females is the same, while it can also be found –in lower concentrations– in the foetus. There is a big difference between species in the route of excretion. In man, rhesus monkey and rabbit it is mostly excreted via the urine, while in rat and dog is was excreted via biliary-faecal excretion. In man and dog, the compound was excreted as the ester glucuronide, and in the other species as the unchanged compound. This means no major metabolic transformation of benoxaprofen takes place.<ref name="Chatfield Disposition">D.H. Chatfield, J.N. Green; Disposition and Metabolism of Benoxaprofen in Laboratory Animals and Man. Lilly Research Centre Limited, Erl Wood Manor, Windlesham, Surrey GU20 6PH, U.K. XENOBIOTICA, 1978, VOL. 8, NO. 3, 133-144</ref>
+In female rats, after oral dose of 20&nbsp;mg/kg, the tissue concentration of benoxaprofen was the highest in liver, kidney, lungs, adrenals and ovaries. The distribution in pregnant females is the same, while it can also be found –in lower concentrations– in the foetus. There is a big difference between species in the route of excretion. In man, rhesus monkey and rabbit it is mostly excreted via the urine, while in rat and dog is was excreted via biliary-faecal excretion. In man and dog, the compound was excreted as the ester glucuronide, and in the other species as the unchanged compound. This means no major metabolic transformation of benoxaprofen takes place.
 ==Toxicodynamics==
-Unlike other non-steroidal anti-inflammatory compounds, benoxaprofen acts directly on mononuclear cells. It inhibits their chemotactic response by inhibiting the [[lipoxygenase]] enzyme.<ref>8.	Benoxaprofen. British Medical Journal London (14 August 1982)</ref>
+Unlike other non-steroidal anti-inflammatory compounds, benoxaprofen acts directly on mononuclear cells. It inhibits their chemotactic response by inhibiting the [[lipoxygenase]] enzyme.
 ==Efficacy and side effects==
 ===Efficacy===
-Benoxaprofen is an [[analgesic]], [[antipyretic]] and anti-inflammatory drug.<ref>Dahl, S.L.; Ward, J.R.: Pharmacology, clinical efficiency, and adverse effects of non-steroidal anti-inflammatory agent benoxaprofen. Abstract</ref>
+Benoxaprofen is an [[analgesic]], [[antipyretic]] and anti-inflammatory drug.
-Benoxaprofen was given to patients with [[rheumatoid arthritis]] and [[osteoarthritis]] because of its anti-inflammatory effect. Patients with the [[Paget's disease of bone|Paget’s disease]], [[psoriatic arthritis]], [[ankylosing spondylitis]], a painful shoulder, the mixed connective-tissue disease, [[polymyalgia rheumatica]], back pain and the [[Behçet’s disease]] received benoxaprofen, too. A daily dose of 300–600&nbsp;mg is effective for many patients.<ref name="Halsey">Halsey, P.; Cardoe, N.: Benaxoprofen: side-effect profile n 300 patients; British medical Journal, Vol 284, pp.1365-1368 (8 May 1982)</ref>
+Benoxaprofen was given to patients with [[rheumatoid arthritis]] and [[osteoarthritis]] because of its anti-inflammatory effect. Patients with the [[Paget's disease of bone|Paget’s disease]], [[psoriatic arthritis]], [[ankylosing spondylitis]], a painful shoulder, the mixed connective-tissue disease, [[polymyalgia rheumatica]], back pain and the [[Behçet’s disease]] received benoxaprofen, too. A daily dose of 300–600&nbsp;mg is effective for many patients.
 ===Adverse effects===
-There are different types of side effects. Most of them were cutaneous or gastrointestinal. Side effects appear rarely in the central nervous system and miscellaneous side effects were not often observed.  A study shows that most side effects appear in patients with rheumatoid arthritis<ref name="Halsey"/>
+There are different types of side effects. Most of them were cutaneous or gastrointestinal. Side effects appear rarely in the central nervous system and miscellaneous side effects were not often observed.  A study shows that most side effects appear in patients with rheumatoid arthritis
 ====Cutaneous side effects====
-Cutaneous side effects of benoxaprofen are [[photosensitivity]], [[onycholysis]], [[rash]], [[milium (disease)|milia]], increased nail growth, [[pruritus]] (itch) and [[hypertrichosis]].<ref name="Halsey"/> Photosensitivity leads to burning, itching or redness when patients are exposed to sunlight.<ref>Hindson, C.; Daymond, T.; Diffey, B.; Lawlor, F.: Side effects of benaxoprofen; Britisch Medical Journal, Vol 284, pp. 1368-1369 (8 May 1982)</ref>
+Cutaneous side effects of benoxaprofen are [[photosensitivity]], [[onycholysis]], [[rash]], [[milium (disease)|milia]], increased nail growth, [[pruritus]] (itch) and [[hypertrichosis]]. Photosensitivity leads to burning, itching or redness when patients are exposed to sunlight.
-A study shows that benoxaprofen, or other lipoxygenase-inhibiting agents, might be helpful in the treatment of [[psoriasis]] because the migration inhibition of the inflammatory cells ([[leukocytes]]) into the skin.<ref>Allen, B.R.; Littlewood, S.M.: Benoxaprofen: effect on cutaneous lesions in psoriasis. British Medical Journal, Vol. 285, p.1241 (30 October 1982)</ref>
+A study shows that benoxaprofen, or other lipoxygenase-inhibiting agents, might be helpful in the treatment of [[psoriasis]] because the migration inhibition of the inflammatory cells ([[leukocytes]]) into the skin.
 ====Gastrointestinal side effects====
-Gastrointestinal side effects of benoxaprofen are bleeding, diarrhoea, abdominal pain, [[anorexia (symptom)]], [[mouth ulcers]] and taste change.<ref name="Halsey"/><ref>Somerville, K.W.; Hawkey, C.J.: Non-steroidal anti-inflammatory agents and the gastrointestinal tract; Postgraduate Medical Journal (1986), Vol 62, pp. 23-28</ref> According to a study the most appearing gastric side effects are vomiting, heartburn and epigastric pain.<ref name="Halsey"/>
+Gastrointestinal side effects of benoxaprofen are bleeding, diarrhoea, abdominal pain, [[anorexia (symptom)]], [[mouth ulcers]] and taste change. According to a study the most appearing gastric side effects are vomiting, heartburn and epigastric pain.
 ====Side effects in the central nervous system====
-For a small number of people, taking benoxaprofen might result in depression, lethargy and feeling ill.<ref name="Halsey"/>
+For a small number of people, taking benoxaprofen might result in depression, lethargy and feeling ill.
 ====Miscellaneous side effects====
-Faintness, dizziness, headache, [[palpitations]], [[epistaxis]], blurred vision, [[urinary urgency]] and [[gynaecomastia]] rarely appear in patients who take benoxaprofen.<ref name="Halsey"/>
+Faintness, dizziness, headache, [[palpitations]], [[epistaxis]], blurred vision, [[urinary urgency]] and [[gynaecomastia]] rarely appear in patients who take benoxaprofen.
-Benoxaprofen also causes [[hepatotoxicity]], which led to death of some elderly patients.<ref>Doube, A.: Hepatitis and non-steroidal anti-flammatory drugs. Animals of the rheumatic diseases (1990), Vol 49, pp. 489-490</ref><ref>McA Taggart, H.; Alderdice, J.M.; Fatal cholestatic jaundice in elderly patients taking benoxaprofen. British Medical Journal, Vol 284, p.1372 ( 8 May 1982)</ref> That was the main reason why the drug was withdrawn from the market.
+Benoxaprofen also causes [[hepatotoxicity]], which led to death of some elderly patients. That was the main reason why the drug was withdrawn from the market.
 ==Toxicity==
-After the suspension of sales in 1982 the toxic effects which benoxaprofen might have on humans were looked into more deeply. The fairly planar compound of benoxaprofen seems to be hepa- and phototoxic in the human body.<ref name="Lewis"/>
+After the suspension of sales in 1982 the toxic effects which benoxaprofen might have on humans were looked into more deeply. The fairly planar compound of benoxaprofen seems to be hepa- and phototoxic in the human body.
-Benoxaprofen has a rather long half life in man (t<sub>1/2</sub>= 20-30 h), undergoes biliary excretion and enterohepatic circulation and is also known to have a slow plasma clearance (CL p=4.5 ml/min). The half life may be further increased in elderly patients (>80 years of age) and in patients which already have an renal impairment increasing to figures as high as 148 hours.<ref name="Lewis"/>
+Benoxaprofen has a rather long half life in man (t<sub>1/2</sub>= 20-30 h), undergoes biliary excretion and enterohepatic circulation and is also known to have a slow plasma clearance (CL p=4.5 ml/min). The half life may be further increased in elderly patients (>80 years of age) and in patients which already have an renal impairment increasing to figures as high as 148 hours.
-The fetal hepatotoxicity of benoxaprofen can be attributed to the accumulation of the drug after a repeated dosage and also associated with the slow plasma clearance. The hepatic accumulation of the drug is presumably the cause for an increase in the activity of the hepatic cytochrome P450I which will oxygenate benaxoprofen and produce reactive intermediates. Benoxaprofen is very likely a substrate and weak inducer of cytochrome P450I and its enzyme family. Normally it is not metabolized by oxidative reactions but with the S(+) enantiomer of benoxaprofen and cytochrome P450I as a catalyst the oxygenation of the 4-chlorophenyl ring and of the aromatic ring of 2-phenyl propionic acid seems to be possible. Therefore the induction of a minor metabolic pathway leads to the formation of toxic metabolites in considerable amounts. The toxic metabolites may bind to vital intracellular macromolecules and may generate reactive oxygens by redox cycling if quinone is formed.<ref name="Lewis"/> This could also lead to a depletion of protective glutathione which is responsible for the detoxification of reactive oxygens.<ref>Andrew, D. A. Loannides, C. Parker, D. V. (1991). Induction of the cytochrome P450 I and IV families and peroxisomal proliferation in the liver of rats treated with benoxaprofen. [[Biochemical Pharmacology]], vol. 42, No.1, pp. 109-115</ref>
+The fetal hepatotoxicity of benoxaprofen can be attributed to the accumulation of the drug after a repeated dosage and also associated with the slow plasma clearance. The hepatic accumulation of the drug is presumably the cause for an increase in the activity of the hepatic cytochrome P450I which will oxygenate benaxoprofen and produce reactive intermediates. Benoxaprofen is very likely a substrate and weak inducer of cytochrome P450I and its enzyme family. Normally it is not metabolized by oxidative reactions but with the S(+) enantiomer of benoxaprofen and cytochrome P450I as a catalyst the oxygenation of the 4-chlorophenyl ring and of the aromatic ring of 2-phenyl propionic acid seems to be possible. Therefore the induction of a minor metabolic pathway leads to the formation of toxic metabolites in considerable amounts. The toxic metabolites may bind to vital intracellular macromolecules and may generate reactive oxygens by redox cycling if quinone is formed. This could also lead to a depletion of protective glutathione which is responsible for the detoxification of reactive oxygens.
-The observed skin phototoxicity of patients treated with benoxaprofen can be explained with a look at the structure of the compound. There are significant structural similarities between the benzoxazole ring of benoxaprofen and the benzafuran ring of psoralen, a compound known to be phototoxic. The free decarboxylated derivate of the drug can produce singlet oxygen and superoxy anions in the presence of oxygen. Furthermore possible explanations for the photochemical decarboxylation and oxygen radical formation may be the accumulation of repeated dosage, the induction of cytochrome P450I and the emergence of reactive intermediates with covalent binding. The photochemical character of the compound can cause inflammation and severe tissue damage.<ref name="Lewis"/>
+The observed skin phototoxicity of patients treated with benoxaprofen can be explained with a look at the structure of the compound. There are significant structural similarities between the benzoxazole ring of benoxaprofen and the benzafuran ring of psoralen, a compound known to be phototoxic. The free decarboxylated derivate of the drug can produce singlet oxygen and superoxy anions in the presence of oxygen. Furthermore possible explanations for the photochemical decarboxylation and oxygen radical formation may be the accumulation of repeated dosage, the induction of cytochrome P450I and the emergence of reactive intermediates with covalent binding. The photochemical character of the compound can cause inflammation and severe tissue damage.
-[[File:Structures benoxaprofen and psoralen.png|thumb|center|upright=2|The structure of psoralen (left) and the structure of benoxaprofen (right). The benzofuran ring and the benoxazole ring are indicated in red.<ref name="Lewis"/>]]
+[[File:Structures benoxaprofen and psoralen.png|none|left|400px]]
-In animals peroxisomal proliferation is also observed but does not seem to be significant in man.<ref name="Lewis"/>
+In animals peroxisomal proliferation is also observed but does not seem to be significant in man.
 ==Effects on animals==
-The effects of Benoxaprofen on animals were tested in a series of experiments.<ref name="Chatfield Disposition"/><ref name="Knights">Knights, K.M. Cassidy, M.R. Drew, R. (1986). Benoxaprofen induced toxicity in isolated rat hepatocytes. Toxicology, Vol.40, p.327-339</ref> Benoxaprofen had a considerably anti-inflammatory, analgesic and also anti-pyretic activity in those tests.<ref name="Chatfield Disposition"/> In all six animals tested, which included rats, dogs, rhesus monkeys, rabbits, guinea pigs and mice, the drug was well absorbed orally. In three of the six species benoxaprofen was then effectively taken up from the gastrointestinal tract (after oral doses of 1–10&nbsp;mg/kg).<ref name="Chatfield Disposition"/> The plasma half life was found to be different, being less than 13 hours in the dog, rabbit and monkey, it was notable longer in mice. Furthermore there were species differences found in the rate and route of excretion of the compound. Whereas benoxaprofen was excreted into the urine by the rabbit and guinea pig, biliary excretion was the way of clearance found in rats and dogs. In all species only unchanged benoxaprofen was found in the plasma mostly extensively bound to proteins.<ref name="Chatfield Disposition"/>
+The effects of Benoxaprofen on animals were tested in a series of experiments. Benoxaprofen had a considerably anti-inflammatory, analgesic and also anti-pyretic activity in those tests. In all six animals tested, which included rats, dogs, rhesus monkeys, rabbits, guinea pigs and mice, the drug was well absorbed orally. In three of the six species benoxaprofen was then effectively taken up from the gastrointestinal tract (after oral doses of 1–10&nbsp;mg/kg). The plasma half life was found to be different, being less than 13 hours in the dog, rabbit and monkey, it was notable longer in mice. Furthermore there were species differences found in the rate and route of excretion of the compound. Whereas benoxaprofen was excreted into the urine by the rabbit and guinea pig, biliary excretion was the way of clearance found in rats and dogs. In all species only unchanged benoxaprofen was found in the plasma mostly extensively bound to proteins.
-The excretion of the unchanged compound into the bile did occur more slowly in rats. This is interpreted by the authors as evidence that no enterohepatic circulation takes place.<ref name="Chatfield Disposition"/> Another research in rats showed that the plasma membrane of hepatocytes begun to form blebs after administration of benoxaprofen. This is suggested to be due to disturbances in the calcium concentration which is possibly a result of an altered cellular redox state which can have an effect on mitochondrial function and therefore cause disturbances in the calcium concentration.<ref name="Knights"/> In none of the species significant levels of metabolism of benoxaprofen were found to have happened. Only in dogs glucuronide could be found in the bile which is a sure sign of metabolism in that species. Also no differences in distribution of the compound in normal and pregnant rats were found. It was shown in rats that benoxaprofen was distributed into the foetus but with a notable lower concentration than in the maternal tissue.<ref name="Chatfield Disposition"/>
+The excretion of the unchanged compound into the bile did occur more slowly in rats. This is interpreted by the authors as evidence that no enterohepatic circulation takes place. Another research in rats showed that the plasma membrane of hepatocytes begun to form blebs after administration of benoxaprofen. This is suggested to be due to disturbances in the calcium concentration which is possibly a result of an altered cellular redox state which can have an effect on mitochondrial function and therefore cause disturbances in the calcium concentration. In none of the species significant levels of metabolism of benoxaprofen were found to have happened. Only in dogs glucuronide could be found in the bile which is a sure sign of metabolism in that species. Also no differences in distribution of the compound in normal and pregnant rats were found. It was shown in rats that benoxaprofen was distributed into the foetus but with a notable lower concentration than in the maternal tissue.
 ==References==
@@ Line 146: / Line 139: @@
 [[Category:Carboxylic acids]]
 [[Category:Eli Lilly and Company]]
-[[Category:Benzoxazoles]]
 [[Category:Organochlorides]]
 [[Category:Drug]]

v t e Nonsteroidal anti-inflammatory drugs (NSAIDs) (primarily M01A and M02A, also N02BA)
Pyrazolones / Pyrazolidines	Aminophenazone Ampyrone Azapropazone Clofezone Difenamizole Famprofazone Feprazone Kebuzone Metamizole Mofebutazone Morazone Nifenazone Oxyphenbutazone Phenazone Phenylbutazone Propyphenazone Sulfinpyrazone Suxibuzone^‡
Salicylates	Aspirin (acetylsalicylic acid)^# Aloxiprin Benorylate Carbasalate calcium Diflunisal Dipyrocetyl Ethenzamide Guacetisal Magnesium salicylate Methyl salicylate Salsalate Salicin Salicylamide Salicylic acid (salicylate) Sodium salicylate
Acetic acid derivatives and related substances	Aceclofenac Acemetacin Alclofenac Amfenac Bendazac Bromfenac Bumadizone Bufexamac Diclofenac Difenpiramide Etodolac Felbinac Fenclozic acid Fentiazac Indometacin Indometacin farnesil Isoxepac Ketorolac Lonazolac Oxametacin Prodolic acid Proglumetacin Sulindac Tiopinac Tolmetin Zomepirac^†
Oxicams	Ampiroxicam Droxicam Isoxicam Lornoxicam Meloxicam Piroxicam Tenoxicam
Propionic acid derivatives (profens)	Alminoprofen Benoxaprofen^† Carprofen^‡ Dexibuprofen Dexketoprofen Fenbufen Fenoprofen Flunoxaprofen Flurbiprofen Ibuprofen^# Ibuproxam Indoprofen^† Ketoprofen Loxoprofen Miroprofen Naproxen Oxaprozin Pirprofen Suprofen Tarenflurbil Tepoxalin^‡ Tiaprofenic acid Vedaprofen^‡ Zaltoprofen COX-inhibiting nitric oxide donator: Naproxcinod
N-Arylanthranilic acids (fenamates)	Azapropazone Clonixin Etofenamate Flufenamic acid Flunixin Meclofenamic acid Mefenamic acid Morniflumate Niflumic acid Tolfenamic acid Flutiazin
Coxibs	Apricoxib Celecoxib Cimicoxib^‡ Deracoxib^‡ Etoricoxib Firocoxib^‡ Lumiracoxib^† Mavacoxib^‡ Parecoxib Robenacoxib^‡ Rofecoxib^† Valdecoxib^†
Other	Aminopropionitrile Benzydamine Chondroitin sulfate Diacerein Fluproquazone Glucosamine Glycosaminoglycan Hyperforin Nabumetone Nimesulide Oxaceprol Proquazone Superoxide dismutase/Orgotein Tenidap
Items listed in bold indicate initially developed compounds of specific groups. ^#WHO-EM ^†Withdrawn drugs. ^‡Veterinary use medications.

Clinical data

ATC code	M01AE06 (WHO)
Identifiers
IUPAC name 2-[2-(4-chlorophenyl)-1,3-benzoxazol-5-yl]propanoic acid
CAS Number	51234-28-7^N
PubChem CID	39941
DrugBank	DB04812^Y
ChemSpider	36518^Y
UNII	17SZX404IM
ChEBI	CHEBI:76114^N
ChEMBL	ChEMBL340978^Y
E number	{{#property:P628}}
ECHA InfoCard	{{#property:P2566}}Lua error in Module:EditAtWikidata at line 36: attempt to index field 'wikibase' (a nil value).
Chemical and physical data
Formula	C₁₆H₁₂ClNO₃
Molar mass	301.72438 g/mol
3D model (JSmol)	Interactive image
SMILES O=C(O)C(c1cc2nc(oc2cc1)c3ccc(Cl)cc3)C
InChI InChI=1S/C16H12ClNO3/c1-9(16(19)20)11-4-7-14-13(8-11)18-15(21-14)10-2-5-12(17)6-3-10/h2-9H,1H3,(H,19,20)^Y Key:MITFXPHMIHQXPI-UHFFFAOYSA-N^Y
^NY (what is this?) (verify)