Parecoxib

Parecoxib
Clinical data
AHFS/Drugs.com	International Drug Names
License data	EU EMA: by INN;
Pregnancy; category	Not recommended;
Routes of; administration	Intravenous and intramuscular
ATC code	M01AH04 (WHO) ;
Legal status
Legal status	AU: S4 (Prescription only) ; UK: POM (Prescription only) ;
Pharmacokinetic data
Bioavailability	100%
Protein binding	98%
Metabolism	Hepatic to valdecoxib and propionic acid; CYP extensively involved (mainly CYP3A4 and 2C9)
Elimination half-life	22 minutes (parecoxib); 8 hours (valdecoxib)
Excretion	Renal (70%, metabolites)
Identifiers
	IUPAC name N-{[4-(5-methyl-3-phenylisoxazol-4-yl)phenyl]; sulfonyl}propanamide;
CAS Number	198470-84-7 ;
PubChem CID	119828;
IUPHAR/BPS	2895;
DrugBank	DB08439 ;
ChemSpider	106990 ;
UNII	9TUW81Y3CE;
ChEBI	CHEBI:73038 ;
ChEMBL	ChEMBL1206690 ;
CompTox Dashboard (EPA)	DTXSID1044229 ;
ECHA InfoCard	100.230.078
Chemical and physical data
Formula	C19H18N2O4S
Molar mass	370.42 g·mol−1
3D model (JSmol)	Interactive image;
	SMILES O=C(NS(=O)(=O)c3ccc(c2c(onc2c1ccccc1)C)cc3)CC;
	InChI InChI=1S/C19H18N2O4S/c1-3-17(22)21-26(23,24)16-11-9-14(10-12-16)18-13(2)25-20-19(18)15-7-5-4-6-8-15/h4-12H,3H2,1-2H3,(H,21,22) ; Key:TZRHLKRLEZJVIJ-UHFFFAOYSA-N ;
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Parecoxib, sold under the brand name Dynastat among others, is a water-soluble and injectable prodrug of valdecoxib. Parecoxib is a COX2 selective inhibitor. It is injectable. It is approved through much of Europe for short term perioperative pain control.

It was patented in 1996 and approved for medical use in 2002.^[1]

Approval[]

In 2005, the U.S. Food and Drug Administration (FDA) issued a letter of non-approval for parecoxib in the United States. No reasons were ever documented publicly for the non-approval, although one study noted increased occurrences of heart attacks following cardiac bypass surgery compared to placebo when high doses of parecoxib were used to control pain after surgery. Importantly, rare but severe allergic reactions (Stevens–Johnson syndrome, Lyell syndrome) have been described with valdecoxib, the molecule to which parecoxib is converted.^[2] The drug is not approved for use after cardiac surgery in Europe.

All anti-inflammatory medications in the U.S. carry the same warning regarding skin reactions, and none are approved for use during CABG surgery, so the reason for the FDA denying the approval of parecoxib remains unknown, but was likely related to political pressure from the US Congress to not approve another COX-2 selective inhibitor in the wake of the Vioxx affair. No COX-2 selective inhibitor has been approved in the US since that time, regardless of the safety profile of parecoxib in Europe. Efforts to find out the scientific rationale, or more likely the lack thereof, that the FDA used to justify the non-approval of parecoxib in the USA have proven futile due to secrecy issues.^[3]^[4]

The political motivation to not approve parecoxib was further supported by a 2017 pooled analysis of safety data in 28 published studies, which showed after 69,567,300 units of parecoxib, skin rash and cardiac complications were minimal, if at all, different from placebo.^[5]

Parecoxib, along with other COX-2 selective inhibitors, celecoxib, valdecoxib, and mavacoxib, were discovered by a team at the Searle division of Monsanto led by John Talley.^[6]^[7]

Parecoxib is the first parenteral COX-2 selective inhibitor available for clinical use in pain management. It is well known from previous clinical trials that its peak serum concentrations occur about thirty minutes after intravenous (IV) administration and one hour after intramuscular (IM) injection. Its first perceptible analgesic effect occurs within seven to thirteen minutes, with clinically meaningful analgesia demonstrated within twenty-three to thirty-nine minutes and a peak effect within two hours following administration of single doses of 40 mg by IV or IM injection.^[8]

References[]

^ Fischer J, Ganellin CR (2006). Analogue-based Drug Discovery. John Wiley & Sons. p. 522. ISBN 9783527607495.
^ Health "Association of Bextra (Valdecoxib) with Serious Adverse Drug Reactions". Health Canada. April 21, 2005.
^ Gajraj NM (2007). "COX-2 inhibitors celecoxib and parecoxib: valuable options for postoperative pain management". Current Topics in Medicinal Chemistry. 7 (3): 235–49. doi:10.2174/156802607779941323. PMID 17305567.
^ Kiehl S (March 13, 2005). "Secrecy on the Rise". The Baltimore Sun.
^ Schug SA, Parsons B, Li C, Xia F (2017). "The safety profile of parecoxib for the treatment of postoperative pain: a pooled analysis of 28 randomized, double-blind, placebo-controlled clinical trials and a review of over 10 years of postauthorization data". Journal of Pain Research. 10: 2451–2459. doi:10.2147/jpr.s136052. PMC 5644539. PMID 29066931.
^ Langreth R (June 23, 2003). "The Chemical Cobbler". Forbes.
^ "Dr. John Talley: 2001 St. Louis Awardee" (PDF). Chemical Bond. St. Louis Section, American Chemical Society. 52 (5): 2. May 2001. Archived from the original (PDF) on 15 April 2018.
^ Mulita, Francesk; Karpetas, Georgios; Liolis, Elias; Vailas, Michail; Tchabashvili, Levan; Maroulis, Ioannis (2021). "Comparison of analgesic efficacy of acetaminophen monotherapy versus acetaminophen combinations with either pethidine or parecoxib in patients undergoing laparoscopic cholecystectomy: a randomized prospective study". Medicinski Glasnik Ljekarske komore Zenicko-dobojskog kantona. 18 (1). doi:10.17392/1245-21. ISSN 1840-0132. PMID 33155461.

v t Non-steroidal 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 Bufexamac Bumadizone Diclofenac Difenpiramide Etodolac Felbinac Fenclozic acid Fentiazac Indometacin Indometacin farnesil Ketorolac Lonazolac Mofezolac Oxametacin Proglumetacin Sulindac 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 Piketoprofen Pirprofen Suprofen Tarenflurbil Tepoxalin^‡ Tiaprofenic acid Vedaprofen^‡ Zaltoprofen COX-inhibiting nitric oxide donator: Naproxcinod
n-arylanthranilic acids (fenamates)	Azapropazone Clonixin Etofenamate Floctafenine Flufenamic acid Flunixin Glafenine^† Meclofenamic acid Mefenamic acid Morniflumate Niflumic acid Tolfenamic acid
COX-2 inhibitors (coxibs)	Apricoxib Celecoxib (+tramadol) 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
NSAID combinations	Ibuprofen/famotidine Ibuprofen/hydrocodone Ibuprofen/oxycodone Ibuprofen/paracetamol Meloxicam/bupivacaine Naproxen/diphenhydramine Naproxen/esomeprazole
Key: underline indicates initially developed first-in-class compound of specific group; ^#WHO-Essential Medicines; ^†withdrawn drugs; ^‡veterinary use.
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Parecoxib

Contents

Approval[]

See also[]

References[]

Further reading[]