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Wikipedia

Clopidogrel

October 20, 2023

Not to be confused with Clopidol.

Clopidogrel — sold under the brand name Plavix, among others[2] — is an antiplatelet medication used to reduce the risk of heart disease and stroke in those at high risk.[5] It is also used together with aspirin in heart attacks and following the placement of a coronary artery stent (dual antiplatelet therapy).[5] It is taken by mouth.[5] Its effect starts about two hours after intake and lasts for five days.[5]

Clopidogrel
Clinical data
Pronunciation/kləˈpɪdəɡrɛl, kl-/[1]
Trade namesPlavix, Iscover, others[2]
AHFS/Drugs.comMonograph
MedlinePlusa601040
License data
Pregnancy
category
Routes of
administration		By mouth
ATC code
Legal status
Legal status
  • AU: S4 (Prescription only)
  • UK: POM (Prescription only)
  • US: ℞-only[4]
  • EU: Rx-only
Pharmacokinetic data
Bioavailability>50%
Protein binding94–98%
MetabolismLiver
Onset of action2 hours[5]
Elimination half-life7–8 hours (inactive metabolite)
Duration of action5 days[5]
Excretion50% Kidney
46% bile duct
Identifiers
  • (+)-(S)-methyl 2-(2-chlorophenyl)-2-(6,7-dihydrothieno[3,2-c]pyridin-5(4H)-yl)acetate
CAS Number
  • 113665-84-2 Y
PubChem CID
  • 60606
IUPHAR/BPS
  • 7150
DrugBank
  • DB00758 Y
ChemSpider
  • 54632 Y
UNII
  • A74586SNO7
KEGG
  • D07729 Y
  • D00769 Y
ChEBI
  • CHEBI:37941 Y
ChEMBL
  • ChEMBL1771 Y
PDB ligand
  • CGE (PDBe, RCSB PDB)
CompTox Dashboard (EPA)
  • DTXSID6022848
ECHA InfoCard100.127.841
Chemical and physical data
FormulaC16H16ClNO2S
Molar mass321.82 g·mol−1
3D model (JSmol)
  • Interactive image
  • COC(=O)[C@H](c1ccccc1Cl)N2CCc3c(ccs3)C2
  • InChI=1S/C16H16ClNO2S/c1-20-16(19)15(12-4-2-3-5-13(12)17)18-8-6-14-11(10-18)7-9-21-14/h2-5,7,9,15H,6,8,10H2,1H3/t15-/m0/s1 Y
  • Key:GKTWGGQPFAXNFI-HNNXBMFYSA-N Y
  (verify)

Common side effects include headache, nausea, easy bruising, itching, and heartburn.[5] More severe side effects include bleeding and thrombotic thrombocytopenic purpura.[5] While there is no evidence of harm from use during pregnancy, such use has not been well studied.[3] Clopidogrel is in the thienopyridine-class of antiplatelets.[5] It works by irreversibly inhibiting a receptor called P2Y12 on platelets.[5]

Clopidogrel was patented in 1982, and approved for medical use in 1997.[4][6] It is on the World Health Organization's List of Essential Medicines.[7] In 2020, it was the 29th most commonly prescribed medication in the United States, with more than 19 million prescriptions.[8][9] It is available as a generic medication.[5]

Medical uses Edit

Clopidogrel is used to prevent heart attack and stroke in people who are at high risk of these events, including those with a history of myocardial infarction and other forms of acute coronary syndrome, stroke, and those with peripheral artery disease.

Treatment with clopidogrel or a related drug is recommended by the American Heart Association and the American College of Cardiology for people who:

  • Present for treatment with a myocardial infarction with ST-elevation[10] including
  • Including a loading dose and maintenance therapy in those receiving PCI and unable to tolerate aspirin therapy
  • Maintenance therapy for up to 12 months in those at medium to high risk for which a noninvasive treatment strategy is chosen
  • In those with stable ischemic heart disease, treatment with clopidogrel is described as a "reasonable" option for monotherapy in those who cannot tolerate aspirin, as is treatment with clopidogrel in combination with aspirin in certain high risk patients.[12]

It is also used, along with acetylsalicylic acid (ASA, aspirin), for the prevention of thrombosis after placement of a coronary stent[13] or as an alternative antiplatelet drug for people intolerant to aspirin.[14] It is available as a fixed-dose combination.[15]

A meta-analysis found clopidogrel's benefit as an antiplatelet drug in reducing cardiovascular death, myocardial infarction, and stroke to be 25% benefit in smokers, with little (8%) benefit in non-smokers.[16]

Consensus-based therapeutic guidelines also recommend the use of clopidogrel rather than aspirin (ASA) for antiplatelet therapy in people with a history of gastric ulceration, as inhibition of the synthesis of prostaglandins by ASA can exacerbate this condition. In people with healed ASA-induced ulcers, however, those receiving ASA plus the proton-pump inhibitor (PPI) esomeprazole had a lower incidence of recurrent ulcer bleeding than those receiving clopidogrel.[17] However, prophylaxis with proton-pump inhibitors along with clopidogrel following acute coronary syndrome may increase adverse cardiac outcomes, possibly due to inhibition of CYP2C19, which is required for the conversion of clopidogrel to its active form.[18][19][20] The European Medicines Agency has issued a public statement on a possible interaction between clopidogrel and proton-pump inhibitors.[21] However, several cardiologists have voiced concern that the studies on which these warnings are based have many limitations and that it is not certain whether an interaction between clopidogrel and proton-pump inhibitors is real.[22]

Adverse effects Edit

Serious adverse drug reactions associated with clopidogrel therapy include:

In the CURE trial, people with acute coronary syndrome without ST elevation were treated with aspirin plus either clopidogrel or placebo and followed for up to one year. The following rates of major bleed were seen:[4]

  • Any major bleeding: clopidogrel 3.7%, placebo 2.7%
  • Life-threatening bleeding: clopidogrel 2.2%, placebo 1.8%
  • Hemorrhagic stroke: clopidogrel 0.1%, placebo 0.1%

The CAPRIE trial compared clopidogrel monotherapy to aspirin monotherapy for 1.6 years in people who had recently experienced a stroke or heart attack. In this trial the following rates of bleeding were observed.[4]

  • Gastrointestinal hemorrhage: clopidogrel 2.0%, aspirin 2.7%
  • Intracranial bleeding: clopidogrel 0.4%, aspirin 0.5%

In CAPRIE, itching was the only adverse effect seen more frequently with clopidogrel than aspirin. In CURE, there was no difference in the rate of non-bleeding adverse events.[4]

Rashes and itching were uncommon in studies (between 0.1 and 1% of people); serious hypersensitivity reactions are rare.[25]

Interactions Edit

Clopidogrel generally has a low potential to interact with other pharmaceutical drugs. Combination with other drugs that affect blood clotting, such as aspirin, heparins and thrombolytics, showed no relevant interactions. Naproxen did increase the likelihood of occult gastrointestinal bleeding, as might be the case with other nonsteroidal anti-inflammatory drugs. As clopidogrel inhibits the liver enzyme CYP2C19 in cellular models, it has been theorized that it might increase blood plasma levels of drugs that are metabolized by this enzyme, such as phenytoin and tolbutamide. Clinical studies showed that this mechanism is irrelevant for practical purposes.[25]

In November 2009, the U.S. Food and Drug Administration (FDA) announced that clopidogrel should be used with caution in people using the proton-pump inhibitors omeprazole or esomeprazole,[26][27][28] but pantoprazole appears to be safe.[29] The newer antiplatelet agent prasugrel has minimal interaction with (es)omeprazole, hence might be a better antiplatelet agent (if no other contraindications are present) in people who are on these proton-pump inhibitors.[30]

Pharmacology Edit

Clopidogrel is a prodrug which is metabolized by the liver into its active form. The active form specifically and irreversibly inhibits the P2Y12 subtype of ADP receptor, which is important in activation of platelets and eventual cross-linking by the protein fibrin.[31]

Pharmacokinetics and metabolism Edit

 
Clopidogrel (top left) being activated: The first step is an oxidation mediated (mainly) by the enzyme CYP2C19, unlike the activation of the related drug prasugrel. The two structures at the bottom are tautomers of each other; and the final step is a hydrolysis. The active metabolite (top right) has Z configuration at the double bond C3–C16 and possibly R configuration at the newly asymmetric C4.[32]

After repeated oral doses of 75 mg of clopidogrel (base), plasma concentrations of the parent compound, which has no platelet-inhibiting effect, are very low and, in general, are below the quantification limit (0.258 µg/L) beyond two hours after dosing.[medical citation needed]

Clopidogrel is a prodrug, which is activated in two steps, first by the enzymes CYP2C19, CYP1A2 and CYP2B6, then by CYP2C19, CYP2C9, CYP2B6 and CYP3A.[31] Due to opening of the thiophene ring, the chemical structure of the active metabolite has three sites that are stereochemically relevant, making a total of eight possible isomers. These are: a stereocentre at C4 (attached to the —SH thiol group), a double bond at C3—C16, and the original stereocentre at C7. Only one of the eight structures is an active antiplatelet drug. This has the following configuration: Z configuration at the C3—C16 double bond, the original S configuration at C7,[32] and, although the stereocentre at C4 cannot be directly determined, as the thiol group is too reactive, work with the active metabolite of the related drug prasugrel suggests the R-configuration of the C4 group is critical for P2Y12 and platelet-inhibitory activity.[medical citation needed]

The active metabolite has an elimination half-life of about 0.5 to 1.0 h, and acts by forming a disulfide bridge with the platelet ADP receptor. Patients with a variant allele of CYP2C19 are 1.5 to 3.5 times more likely to die or have complications than patients with the high-functioning allele.[33][34][35]

Following an oral dose of 14C-labeled clopidogrel in humans, about 50% was excreted in the urine and 46% in the feces in the five days after dosing.[5]

  • Effect of food: Administration of clopidogrel bisulfate with meals did not significantly modify the bioavailability of clopidogrel as assessed by the pharmacokinetics of the main circulating metabolite.
  • Absorption and distribution: Clopidogrel is rapidly absorbed after oral administration of repeated doses of 75-milligram clopidogrel (base), with peak plasma levels (about 3 mg/L) of the main circulating metabolite occurring around one hour after dosing. The pharmacokinetics of the main circulating metabolite are linear (plasma concentrations increased in proportion to dose) in the dose range of 50 to 150 mg of clopidogrel. Absorption is at least 50% based on urinary excretion of clopidogrel-related metabolites.

Clopidogrel and the main circulating metabolite bind reversibly in vitro to human plasma proteins (98% and 94%, respectively). The binding is not saturable in vitro up to a concentration of 110 μg/mL.

  • Metabolism and elimination: In vitro and in vivo, clopidogrel undergoes rapid hydrolysis into its carboxylic acid derivative. In plasma and urine, the glucuronide of the carboxylic acid derivative is also observed.

In 2010 the U.S. Food and Drug Administration (FDA) added a boxed warning, later updated, to Plavix, alerting that the drug can be less effective in people unable to metabolize the drug to convert it to its active form.[36]

Pharmacogenetics Edit

CYP2C19 is an important drug-metabolizing enzyme that catalyzes the biotransformation of many clinically useful drugs, including antidepressants, barbiturates, proton-pump inhibitors, and antimalarial and antitumor drugs. Clopidogrel is one of the drugs metabolized by this enzyme.[5]

The U.S. Food and Drug Administration (FDA) put a black box warning on Plavix in 2010, later updated, to make patients and healthcare providers aware that CYP2C19-poor metabolizers, representing up to 14% of patients, are at high risk of treatment failure and that testing is available.[36] Patients with variants in cytochrome P-450 2C19 (CYP2C19) have lower levels of the active metabolite of clopidogrel, less inhibition of platelets, and a 3.58-times greater risk for major adverse cardiovascular events such as death, heart attack, and stroke; the risk was greatest in CYP2C19 poor metabolizers.[4][37]

A published review showed that some mutations of CYP2C19, CYP3A4, CYP2C9, CYP2B6, and CYP1A2 genes could affect the clinical efficacy and safety of clopidogrel treatment. For instance, patients carrying the mutations CYP2C19*2, CYP2C19*3, CYP2C9*2, CYP2C9*3, and CYP2B6*5 alleles may not respond to clopidogrel due to poor platelet inhibition efficacy revealed among them.[38]

Mechanism of action Edit

The active metabolite of clopidogrel specifically and irreversibly inhibits the P2Y12 subtype of ADP receptor, which is important in activation of platelets and eventual cross-linking by the protein fibrin.[31] Platelet inhibition can be demonstrated two hours after a single dose of oral clopidogrel, but the onset of action is slow, so a loading dose of either 600 or 300 mg is administered when a rapid effect is needed.[39][full citation needed]

Society and culture Edit

Economics Edit

 
A box of Plavix

Plavix is marketed worldwide in nearly 110 countries, with sales of US$6.6 billion in 2009.[40] It was the second-top-selling drug in the world in 2007[41] and was still growing by over 20% in 2007. U.S. sales were US$3.8 billion in 2008.[42]

Before the expiry of its patent, clopidogrel was the second best-selling drug in the world. In 2010, it grossed over US$9 billion in global sales.[43]

In 2006, generic clopidogrel was briefly marketed by Apotex, a Canadian generic pharmaceutical company before a court order halted further production until resolution of a patent infringement case brought by Bristol-Myers Squibb.[44] The court ruled that Bristol-Myers Squibb's patent was valid and provided protection until November 2011.[45] The FDA extended the patent protection of clopidogrel by six months, giving exclusivity that would expire on 17 May 2012.[46] The FDA approved generic versions of Plavix on 17 May 2012.[47]

Names Edit

Generic clopidogrel is marketed by many companies worldwide under many brand names.[2]

List of brand names

As of March 2017, brands included Aclop, Actaclo, Agregex, Agrelan, Agrelax, Agreless, Agrelex, Agreplat, Anclog, Angiclod, Anplat, Antiagrex, Antiban, Antigrel, Antiplaq, Antiplar, Aplate, Apolets, Areplex, Artepid, Asogrel, Atelit, Atelit, Ateplax, Atervix, Atheros, Athorel, Atrombin, Attera, Bidogrel, Bigrel, Borgavix, Carder, Cardogrel, Carpigrel, Ceraenade, Ceruvin, Cidorix, Clatex, Clavix, Clentel, Clentel, Clidorel, Clodel, Clodelib, Clodian, Clodil, Cloflow, Clofre, Clogan, Clogin, Clognil, Clogrel, Clogrelhexal, Clolyse, Clont, Clood, Clopacin, Clopcare, Clopeno, Clopex Agrel, Clopez, Clopi, Clopid, Clopida, Clopidep, Clopidexcel, Clopidix, Clopidogrel, Clopidogrelum, Clopidomed, Clopidorex, Clopidosyn, Clopidoteg, Clopidowel, Clopidra, Clopidrax, Clopidrol, Clopigal, Clopigamma, Clopigrel, Clopilet, Clopimed, Clopimef, Clopimet, Clopinovo, Clopione, Clopiright, Clopirite, Clopirod, Clopisan, Clopistad, Clopistad, Clopitab, Clopithan, Clopitro, ClopiVale, Clopivas, Clopivaz, Clopivid, Clopivin, Clopix, Cloplat, Clopra, Cloprez, Cloprez, Clopval, Clorel, Cloriocard, Cloroden, Clotix, Clotiz, Clotrombix, Clova, Clovas, Clovax, Clovelen, Clovex, Clovexil, Clovix, Clovvix, Copalex, Copegrel, Copidrel, Copil, Cordiax, Cordix, Corplet, Cotol, CPG, Cugrel, Curovix, Dapixol, Darxa, Dasogrel-S, Dclot, Defrozyp, Degregan, Deplat, Deplatt, Diclop, Diloxol, Dilutix, Diporel, Doglix, Dogrel, Dogrel, Dopivix, Dorel, Dorell, Duopidogrel, DuoPlavin, Eago, Egitromb, Espelio, Eurogrel, Expansia, Farcet, Flucogrel, Fluxx, Freeclo, Globel, Glopenel, Grelet, Greligen, Grelix, Grepid, Grepid, Grindokline, Heart-Free, Hemaflow, Hyvix, Idiavix, Insigrel, Iscover, Iskimil, Kafidogran, Kaldera, Kardogrel, Karum, Kerberan, Keriten, Klepisal, Klogrel, Klopide, Klopidex, Klopidogrel, Klopik, Klopis, Kogrel, Krossiler, Larvin, Lodigrel, Lodovax, Lofradyk, Lopigalel, Lopirel, Lyvelsa, Maboclop, Medigrel, Miflexin, Mistro, Mogrel, Monel, Monogrel, Moytor, Myogrel, Nabratin, Nadenel, Nefazan, Niaclop, Nivenol, Noclog, Nofardom, Nogreg, Nogrel, Noklot, Norplat, Novigrel, Oddoral, Odrel, Olfovel, Opirel, Optigrel, Panagrel, Pedovex, Pegorel, Piax, Piclokare, Pidgrel, Pidogrel, Pidogul, Pidovix, Pigrel, Pingel, Placta, Pladel, Pladex, Pladogrel, Plagerine, Plagrel, Plagril, Plagrin, Plahasan, Plamed, Planor, PlaquEx, Plasiver, Plataca, Platarex, Platec, Platel, Platelex, Platexan, Platil, Platless, Platogrix, Platrel, Plavedamol, Plavicard, Plavictonal, Plavidosa, Plavigrel, Plavihex, Plavitor, Plavix, Plavocorin, Plavogrel, Plavos, Pleyar, Plogrel, Plvix, Pravidel, Pregrel, Provic, Psygrel, Q.O.L, Ravalgen, Replet, Respekt, Revlis, Ridlor, Roclas, Rozak, Sanvix, Sarix, Sarovex, Satoxi, Shinclop, Sigmagrel, Simclovix, Sintiplex, Stazex, Stroka, Stromix, Sudroc, Synetra, Talcom, Tansix, Tessyron, Thinrin, Throimper, Thrombifree, Thrombo, Timiflo, Tingreks, Torpido, Triosal, Trogran, Troken, Trombex, Trombix, Tuxedon, Unigrel, Unplaque, Vaclo, Vasocor, Vatoud, Venicil, Vidogrel, Vivelon, Vixam, Xydrel, Zakogrel, Zillt, Zopya, Zylagren, Zyllt, and Zystol.[2]

As of 2017, it was marketed as a combination drug with acetylsalicylic acid (aspirin) under the brand names Anclog Plus, Antiban-ASP, Asclop, Asogrel-A, Aspin-Plus, Cargrel-A, Clas, Clasprin, Clavixin Duo, Clodrel Forte, Clodrel Plus, Clofre AS, Clognil Plus, Clontas, Clopid-AS, Clopid-AS, Clopida A, Clopil-A, Clopirad-A, Clopirin, Clopitab-A, Clorel-A, Clouds, Combiplat, Coplavix, Coplavix, Cugrel-A, Dorel Plus, DuoCover, DuoCover, DuoPlavin, DuoPlavin, Ecosprin Plus, Grelet-A, Lopirel Plus, Myogrel-AP, Noclog Plus, Noklot Plus, Norplat-S, Odrel Plus, Pidogul A, Pladex-A, Plagerine-A, Plagrin Plus, Plavix Plus, Replet Plus, Stromix-A, and Thrombosprin.[2]

Veterinary uses Edit

Clopidogrel has been shown to be effective at decreasing platelet aggregation in cats, so its use in prevention of feline aortic thromboembolism has been advocated.[48]

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  37. ^ "FDA Drug Safety Communication: Reduced effectiveness of Plavix (clopidogrel) in patients who are poor metabolizers of the drug". U.S. Food and Drug Administration (FDA). 28 June 2019. from the original on 18 June 2019. Retrieved 30 January 2022.
  38. ^ Alkattan A, Alsalameen E (June 2021). "Polymorphisms of genes related to phase-I metabolic enzymes affecting the clinical efficacy and safety of clopidogrel treatment". Expert Opinion on Drug Metabolism & Toxicology. 17 (6): 685–95. doi:10.1080/17425255.2021.1925249. PMID 33931001. S2CID 233470717.
  39. ^ Clopidogrel Multum Consumer Information
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  48. ^ Hogan DF, Andrews DA, Green HW, et al. (2004). "Antiplatelet effects and pharmacodynamics of clopidogrel in cats". J Am Vet Med Assoc. 225 (9): 1406–1411. doi:10.2460/javma.2004.225.1406. PMID 15552317.

Further reading Edit

External links Edit

  • "Clopidogrel". Drug Information Portal. U.S. National Library of Medicine.
  • US Patent US4847265A for "Dextro-rotatory enantiomer of methyl alpha-5 (4,5,6,7-tetrahydro (3,2-c) thieno pyridyl) (2-chlorophenyl)-acetate and the pharmaceutical compositions containing it"

October 20, 2023
clopidogrel, confused, with, clopidol, sold, under, brand, name, plavix, among, others, antiplatelet, medication, used, reduce, risk, heart, disease, stroke, those, high, risk, also, used, together, with, aspirin, heart, attacks, following, placement, coronary. Not to be confused with Clopidol Clopidogrel sold under the brand name Plavix among others 2 is an antiplatelet medication used to reduce the risk of heart disease and stroke in those at high risk 5 It is also used together with aspirin in heart attacks and following the placement of a coronary artery stent dual antiplatelet therapy 5 It is taken by mouth 5 Its effect starts about two hours after intake and lasts for five days 5 ClopidogrelClinical dataPronunciation k l e ˈ p ɪ d e ɡ r ɛ l k l oʊ 1 Trade namesPlavix Iscover others 2 AHFS Drugs comMonographMedlinePlusa601040License dataEU EMA by INN US DailyMed Clopidogrel US FDA ClopidogrelPregnancycategoryAU B1 3 Routes ofadministrationBy mouthATC codeB01AC04 WHO Legal statusLegal statusAU S4 Prescription only UK POM Prescription only US only 4 EU Rx onlyPharmacokinetic dataBioavailability gt 50 Protein binding94 98 MetabolismLiverOnset of action2 hours 5 Elimination half life7 8 hours inactive metabolite Duration of action5 days 5 Excretion50 Kidney46 bile ductIdentifiersIUPAC name S methyl 2 2 chlorophenyl 2 6 7 dihydrothieno 3 2 c pyridin 5 4H yl acetateCAS Number113665 84 2 YPubChem CID60606IUPHAR BPS7150DrugBankDB00758 YChemSpider54632 YUNIIA74586SNO7KEGGD07729 YD00769 YChEBICHEBI 37941 YChEMBLChEMBL1771 YPDB ligandCGE PDBe RCSB PDB CompTox Dashboard EPA DTXSID6022848ECHA InfoCard100 127 841Chemical and physical dataFormulaC 16H 16Cl N O 2SMolar mass321 82 g mol 13D model JSmol Interactive imageSMILES COC O C H c1ccccc1Cl N2CCc3c ccs3 C2InChI InChI 1S C16H16ClNO2S c1 20 16 19 15 12 4 2 3 5 13 12 17 18 8 6 14 11 10 18 7 9 21 14 h2 5 7 9 15H 6 8 10H2 1H3 t15 m0 s1 YKey GKTWGGQPFAXNFI HNNXBMFYSA N Y verify Common side effects include headache nausea easy bruising itching and heartburn 5 More severe side effects include bleeding and thrombotic thrombocytopenic purpura 5 While there is no evidence of harm from use during pregnancy such use has not been well studied 3 Clopidogrel is in the thienopyridine class of antiplatelets 5 It works by irreversibly inhibiting a receptor called P2Y12 on platelets 5 Clopidogrel was patented in 1982 and approved for medical use in 1997 4 6 It is on the World Health Organization s List of Essential Medicines 7 In 2020 it was the 29th most commonly prescribed medication in the United States with more than 19 million prescriptions 8 9 It is available as a generic medication 5 Contents 1 Medical uses 2 Adverse effects 3 Interactions 4 Pharmacology 4 1 Pharmacokinetics and metabolism 4 2 Pharmacogenetics 4 3 Mechanism of action 5 Society and culture 5 1 Economics 5 2 Names 6 Veterinary uses 7 References 8 Further reading 9 External linksMedical uses EditClopidogrel is used to prevent heart attack and stroke in people who are at high risk of these events including those with a history of myocardial infarction and other forms of acute coronary syndrome stroke and those with peripheral artery disease Treatment with clopidogrel or a related drug is recommended by the American Heart Association and the American College of Cardiology for people who Present for treatment with a myocardial infarction with ST elevation 10 includingA loading dose given in advance of percutaneous coronary intervention PCI followed by a full year of treatment for those receiving a vascular stent A loading dose given in advance of fibrinolytic therapy continued for at least 14 daysPresent for treatment of a non ST elevation myocardial infarction or unstable angina 11 Including a loading dose and maintenance therapy in those receiving PCI and unable to tolerate aspirin therapy Maintenance therapy for up to 12 months in those at medium to high risk for which a noninvasive treatment strategy is chosenIn those with stable ischemic heart disease treatment with clopidogrel is described as a reasonable option for monotherapy in those who cannot tolerate aspirin as is treatment with clopidogrel in combination with aspirin in certain high risk patients 12 It is also used along with acetylsalicylic acid ASA aspirin for the prevention of thrombosis after placement of a coronary stent 13 or as an alternative antiplatelet drug for people intolerant to aspirin 14 It is available as a fixed dose combination 15 A meta analysis found clopidogrel s benefit as an antiplatelet drug in reducing cardiovascular death myocardial infarction and stroke to be 25 benefit in smokers with little 8 benefit in non smokers 16 Consensus based therapeutic guidelines also recommend the use of clopidogrel rather than aspirin ASA for antiplatelet therapy in people with a history of gastric ulceration as inhibition of the synthesis of prostaglandins by ASA can exacerbate this condition In people with healed ASA induced ulcers however those receiving ASA plus the proton pump inhibitor PPI esomeprazole had a lower incidence of recurrent ulcer bleeding than those receiving clopidogrel 17 However prophylaxis with proton pump inhibitors along with clopidogrel following acute coronary syndrome may increase adverse cardiac outcomes possibly due to inhibition of CYP2C19 which is required for the conversion of clopidogrel to its active form 18 19 20 The European Medicines Agency has issued a public statement on a possible interaction between clopidogrel and proton pump inhibitors 21 However several cardiologists have voiced concern that the studies on which these warnings are based have many limitations and that it is not certain whether an interaction between clopidogrel and proton pump inhibitors is real 22 Adverse effects EditSerious adverse drug reactions associated with clopidogrel therapy include Thrombotic thrombocytopenic purpura incidence four per million patients treated 23 4 Hemorrhage the annual incidence of hemorrhage may be increased by the coadministration of aspirin 24 In the CURE trial people with acute coronary syndrome without ST elevation were treated with aspirin plus either clopidogrel or placebo and followed for up to one year The following rates of major bleed were seen 4 Any major bleeding clopidogrel 3 7 placebo 2 7 Life threatening bleeding clopidogrel 2 2 placebo 1 8 Hemorrhagic stroke clopidogrel 0 1 placebo 0 1 The CAPRIE trial compared clopidogrel monotherapy to aspirin monotherapy for 1 6 years in people who had recently experienced a stroke or heart attack In this trial the following rates of bleeding were observed 4 Gastrointestinal hemorrhage clopidogrel 2 0 aspirin 2 7 Intracranial bleeding clopidogrel 0 4 aspirin 0 5 In CAPRIE itching was the only adverse effect seen more frequently with clopidogrel than aspirin In CURE there was no difference in the rate of non bleeding adverse events 4 Rashes and itching were uncommon in studies between 0 1 and 1 of people serious hypersensitivity reactions are rare 25 Interactions EditClopidogrel generally has a low potential to interact with other pharmaceutical drugs Combination with other drugs that affect blood clotting such as aspirin heparins and thrombolytics showed no relevant interactions Naproxen did increase the likelihood of occult gastrointestinal bleeding as might be the case with other nonsteroidal anti inflammatory drugs As clopidogrel inhibits the liver enzyme CYP2C19 in cellular models it has been theorized that it might increase blood plasma levels of drugs that are metabolized by this enzyme such as phenytoin and tolbutamide Clinical studies showed that this mechanism is irrelevant for practical purposes 25 In November 2009 the U S Food and Drug Administration FDA announced that clopidogrel should be used with caution in people using the proton pump inhibitors omeprazole or esomeprazole 26 27 28 but pantoprazole appears to be safe 29 The newer antiplatelet agent prasugrel has minimal interaction with es omeprazole hence might be a better antiplatelet agent if no other contraindications are present in people who are on these proton pump inhibitors 30 Pharmacology EditClopidogrel is a prodrug which is metabolized by the liver into its active form The active form specifically and irreversibly inhibits the P2Y12 subtype of ADP receptor which is important in activation of platelets and eventual cross linking by the protein fibrin 31 Pharmacokinetics and metabolism Edit nbsp Clopidogrel top left being activated The first step is an oxidation mediated mainly by the enzyme CYP2C19 unlike the activation of the related drug prasugrel The two structures at the bottom are tautomers of each other and the final step is a hydrolysis The active metabolite top right has Z configuration at the double bond C3 C16 and possibly R configuration at the newly asymmetric C4 32 After repeated oral doses of 75 mg of clopidogrel base plasma concentrations of the parent compound which has no platelet inhibiting effect are very low and in general are below the quantification limit 0 258 µg L beyond two hours after dosing medical citation needed Clopidogrel is a prodrug which is activated in two steps first by the enzymes CYP2C19 CYP1A2 and CYP2B6 then by CYP2C19 CYP2C9 CYP2B6 and CYP3A 31 Due to opening of the thiophene ring the chemical structure of the active metabolite has three sites that are stereochemically relevant making a total of eight possible isomers These are a stereocentre at C4 attached to the SH thiol group a double bond at C3 C16 and the original stereocentre at C7 Only one of the eight structures is an active antiplatelet drug This has the following configuration Z configuration at the C3 C16 double bond the original S configuration at C7 32 and although the stereocentre at C4 cannot be directly determined as the thiol group is too reactive work with the active metabolite of the related drug prasugrel suggests the R configuration of the C4 group is critical for P2Y12 and platelet inhibitory activity medical citation needed The active metabolite has an elimination half life of about 0 5 to 1 0 h and acts by forming a disulfide bridge with the platelet ADP receptor Patients with a variant allele of CYP2C19 are 1 5 to 3 5 times more likely to die or have complications than patients with the high functioning allele 33 34 35 Following an oral dose of 14C labeled clopidogrel in humans about 50 was excreted in the urine and 46 in the feces in the five days after dosing 5 Effect of food Administration of clopidogrel bisulfate with meals did not significantly modify the bioavailability of clopidogrel as assessed by the pharmacokinetics of the main circulating metabolite Absorption and distribution Clopidogrel is rapidly absorbed after oral administration of repeated doses of 75 milligram clopidogrel base with peak plasma levels about 3 mg L of the main circulating metabolite occurring around one hour after dosing The pharmacokinetics of the main circulating metabolite are linear plasma concentrations increased in proportion to dose in the dose range of 50 to 150 mg of clopidogrel Absorption is at least 50 based on urinary excretion of clopidogrel related metabolites Clopidogrel and the main circulating metabolite bind reversibly in vitro to human plasma proteins 98 and 94 respectively The binding is not saturable in vitro up to a concentration of 110 mg mL Metabolism and elimination In vitro and in vivo clopidogrel undergoes rapid hydrolysis into its carboxylic acid derivative In plasma and urine the glucuronide of the carboxylic acid derivative is also observed In 2010 the U S Food and Drug Administration FDA added a boxed warning later updated to Plavix alerting that the drug can be less effective in people unable to metabolize the drug to convert it to its active form 36 Pharmacogenetics Edit CYP2C19 is an important drug metabolizing enzyme that catalyzes the biotransformation of many clinically useful drugs including antidepressants barbiturates proton pump inhibitors and antimalarial and antitumor drugs Clopidogrel is one of the drugs metabolized by this enzyme 5 The U S Food and Drug Administration FDA put a black box warning on Plavix in 2010 later updated to make patients and healthcare providers aware that CYP2C19 poor metabolizers representing up to 14 of patients are at high risk of treatment failure and that testing is available 36 Patients with variants in cytochrome P 450 2C19 CYP2C19 have lower levels of the active metabolite of clopidogrel less inhibition of platelets and a 3 58 times greater risk for major adverse cardiovascular events such as death heart attack and stroke the risk was greatest in CYP2C19 poor metabolizers 4 37 A published review showed that some mutations of CYP2C19 CYP3A4 CYP2C9 CYP2B6 and CYP1A2 genes could affect the clinical efficacy and safety of clopidogrel treatment For instance patients carrying the mutations CYP2C19 2 CYP2C19 3 CYP2C9 2 CYP2C9 3 and CYP2B6 5 alleles may not respond to clopidogrel due to poor platelet inhibition efficacy revealed among them 38 Mechanism of action Edit The active metabolite of clopidogrel specifically and irreversibly inhibits the P2Y12 subtype of ADP receptor which is important in activation of platelets and eventual cross linking by the protein fibrin 31 Platelet inhibition can be demonstrated two hours after a single dose of oral clopidogrel but the onset of action is slow so a loading dose of either 600 or 300 mg is administered when a rapid effect is needed 39 full citation needed Society and culture EditEconomics Edit nbsp A box of PlavixPlavix is marketed worldwide in nearly 110 countries with sales of US 6 6 billion in 2009 40 It was the second top selling drug in the world in 2007 41 and was still growing by over 20 in 2007 U S sales were US 3 8 billion in 2008 42 Before the expiry of its patent clopidogrel was the second best selling drug in the world In 2010 it grossed over US 9 billion in global sales 43 In 2006 generic clopidogrel was briefly marketed by Apotex a Canadian generic pharmaceutical company before a court order halted further production until resolution of a patent infringement case brought by Bristol Myers Squibb 44 The court ruled that Bristol Myers Squibb s patent was valid and provided protection until November 2011 45 The FDA extended the patent protection of clopidogrel by six months giving exclusivity that would expire on 17 May 2012 46 The FDA approved generic versions of Plavix on 17 May 2012 47 Names Edit Generic clopidogrel is marketed by many companies worldwide under many brand names 2 List of brand namesAs of March 2017 update brands included Aclop Actaclo Agregex Agrelan Agrelax Agreless Agrelex Agreplat Anclog Angiclod Anplat Antiagrex Antiban Antigrel Antiplaq Antiplar Aplate Apolets Areplex Artepid Asogrel Atelit Atelit Ateplax Atervix Atheros Athorel Atrombin Attera Bidogrel Bigrel Borgavix Carder Cardogrel Carpigrel Ceraenade Ceruvin Cidorix Clatex Clavix Clentel Clentel Clidorel Clodel Clodelib Clodian Clodil Cloflow Clofre Clogan Clogin Clognil Clogrel Clogrelhexal Clolyse Clont Clood Clopacin Clopcare Clopeno Clopex Agrel Clopez Clopi Clopid Clopida Clopidep Clopidexcel Clopidix Clopidogrel Clopidogrelum Clopidomed Clopidorex Clopidosyn Clopidoteg Clopidowel Clopidra Clopidrax Clopidrol Clopigal Clopigamma Clopigrel Clopilet Clopimed Clopimef Clopimet Clopinovo Clopione Clopiright Clopirite Clopirod Clopisan Clopistad Clopistad Clopitab Clopithan Clopitro ClopiVale Clopivas Clopivaz Clopivid Clopivin Clopix Cloplat Clopra Cloprez Cloprez Clopval Clorel Cloriocard Cloroden Clotix Clotiz Clotrombix Clova Clovas Clovax Clovelen Clovex Clovexil Clovix Clovvix Copalex Copegrel Copidrel Copil Cordiax Cordix Corplet Cotol CPG Cugrel Curovix Dapixol Darxa Dasogrel S Dclot Defrozyp Degregan Deplat Deplatt Diclop Diloxol Dilutix Diporel Doglix Dogrel Dogrel Dopivix Dorel Dorell Duopidogrel DuoPlavin Eago Egitromb Espelio Eurogrel Expansia Farcet Flucogrel Fluxx Freeclo Globel Glopenel Grelet Greligen Grelix Grepid Grepid Grindokline Heart Free Hemaflow Hyvix Idiavix Insigrel Iscover Iskimil Kafidogran Kaldera Kardogrel Karum Kerberan Keriten Klepisal Klogrel Klopide Klopidex Klopidogrel Klopik Klopis Kogrel Krossiler Larvin Lodigrel Lodovax Lofradyk Lopigalel Lopirel Lyvelsa Maboclop Medigrel Miflexin Mistro Mogrel Monel Monogrel Moytor Myogrel Nabratin Nadenel Nefazan Niaclop Nivenol Noclog Nofardom Nogreg Nogrel Noklot Norplat Novigrel Oddoral Odrel Olfovel Opirel Optigrel Panagrel Pedovex Pegorel Piax Piclokare Pidgrel Pidogrel Pidogul Pidovix Pigrel Pingel Placta Pladel Pladex Pladogrel Plagerine Plagrel Plagril Plagrin Plahasan Plamed Planor PlaquEx Plasiver Plataca Platarex Platec Platel Platelex Platexan Platil Platless Platogrix Platrel Plavedamol Plavicard Plavictonal Plavidosa Plavigrel Plavihex Plavitor Plavix Plavocorin Plavogrel Plavos Pleyar Plogrel Plvix Pravidel Pregrel Provic Psygrel Q O L Ravalgen Replet Respekt Revlis Ridlor Roclas Rozak Sanvix Sarix Sarovex Satoxi Shinclop Sigmagrel Simclovix Sintiplex Stazex Stroka Stromix Sudroc Synetra Talcom Tansix Tessyron Thinrin Throimper Thrombifree Thrombo Timiflo Tingreks Torpido Triosal Trogran Troken Trombex Trombix Tuxedon Unigrel Unplaque Vaclo Vasocor Vatoud Venicil Vidogrel Vivelon Vixam Xydrel Zakogrel Zillt Zopya Zylagren Zyllt and Zystol 2 As of 2017 update it was marketed as a combination drug with acetylsalicylic acid aspirin under the brand names Anclog Plus Antiban ASP Asclop Asogrel A Aspin Plus Cargrel A Clas Clasprin Clavixin Duo Clodrel Forte Clodrel Plus Clofre AS Clognil Plus Clontas Clopid AS Clopid AS Clopida A Clopil A Clopirad A Clopirin Clopitab A Clorel A Clouds Combiplat Coplavix Coplavix Cugrel A Dorel Plus DuoCover DuoCover DuoPlavin DuoPlavin Ecosprin Plus Grelet A Lopirel Plus Myogrel AP Noclog Plus Noklot Plus Norplat S Odrel Plus Pidogul A Pladex A Plagerine A Plagrin Plus Plavix Plus Replet Plus Stromix A and Thrombosprin 2 Veterinary uses EditClopidogrel has been shown to be effective at decreasing platelet aggregation in cats so its use in prevention of feline aortic thromboembolism has been advocated 48 References Edit Clopidogrel Lexico Dictionaries Archived from the original on 25 October 2019 Retrieved 26 October 2019 a b c d e Clopidogrel International brand names Drugs com Archived from the original on 1 April 2017 Retrieved 1 April 2017 a b Clopidogrel Plavix Use During Pregnancy Drugs com Archived from the original on 21 December 2016 Retrieved 14 December 2016 a b c d e f g Plavix clopidogrel bisulfate tablet film coated DailyMed Bristol Myers Squibb Sanofi Pharmaceuticals Partnership 17 May 2019 Archived from the original on 4 August 2020 Retrieved 26 December 2019 a b c d e f g h i j k l m Clopidogrel Bisulfate The American Society of Health System Pharmacists Archived from the original on 21 December 2016 Retrieved 8 December 2016 Fischer J Ganellin CR 2006 Analogue based Drug Discovery John Wiley amp Sons p 453 ISBN 9783527607495 Archived from the original on 20 December 2016 World Health Organization 2019 World Health Organization model list of essential medicines 21st list 2019 Geneva World Health Organization hdl 10665 325771 WHO MVP EMP IAU 2019 06 License CC BY NC SA 3 0 IGO The Top 300 of 2020 ClinCalc Retrieved 7 October 2022 Clopidogrel Drug Usage Statistics ClinCalc Retrieved 7 October 2022 O Gara PT Kushner FG Ascheim DD et al January 2013 2013 ACCF AHA guideline for the management of ST elevation myocardial infarction a report of the American College of Cardiology Foundation American Heart Association Task Force on Practice Guidelines J Am Coll Cardiol 61 4 e78 140 doi 10 1016 j jacc 2012 11 019 PMID 23256914 Jneid H Anderson JL Wright RS et al August 2012 2012 ACCF AHA focused update of the guideline for the management of patients with unstable angina Non ST elevation myocardial infarction updating the 2007 guideline and replacing the 2011 focused update a report of the American College of Cardiology Foundation American Heart Association Task Force on practice guidelines Circulation 126 7 875 910 doi 10 1161 CIR 0b013e318256f1e0 PMID 22800849 Fihn SD Gardin JM Abrams J et al December 2012 2012 ACCF AHA ACP AATS PCNA SCAI STS guideline for the diagnosis and management of patients with stable ischemic heart disease executive summary a report of the American College of Cardiology Foundation American Heart Association task force on practice guidelines and the American College of Physicians American Association for Thoracic Surgery Preventive Cardiovascular Nurses Association Society for Cardiovascular Angiography and Interventions and Society of Thoracic Surgeons Circulation 126 25 3097 137 doi 10 1161 CIR 0b013e3182776f83 PMID 23166210 Rossi S editor Australian Medicines Handbook 2006 Adelaide Australian Medicines Handbook 2006 ISBN 0 9757919 2 3 Michael D Randall Karen E Neil 2004 Disease management 2nd ed London Pharmaceutical Press 159 DuoPlavin EPAR European Medicines Agency EMA 17 September 2018 Archived from the original on 4 September 2020 Retrieved 21 August 2020 Gagne JJ Bykov K Choudhry NK et al 17 September 2013 Effect of smoking on comparative efficacy of antiplatelet agents systematic review meta analysis and indirect comparison BMJ Clinical Research Ed 347 f5307 doi 10 1136 bmj f5307 PMC 3775704 PMID 24046285 Chan FK Ching JY Hung LC et al 2005 Clopidogrel versus aspirin and esomeprazole to prevent recurrent ulcer bleeding N Engl J Med 352 3 238 44 doi 10 1056 NEJMoa042087 PMID 15659723 Mistry SD Trivedi HR Parmar DM et al 2011 Impact of proton pump inhibitors on efficacy of clopidogrel Review of evidence Indian Journal of Pharmacology 43 2 183 6 doi 10 4103 0253 7613 77360 PMC 3081459 PMID 21572655 Ho PM Maddox TM Wang L et al 2009 Risk of adverse outcomes associated with concomitant use of clopidogrel and proton pump inhibitors following acute coronary syndrome Journal of the American Medical Association 301 9 937 44 doi 10 1001 jama 2009 261 PMID 19258584 Stockl KM Le L Zakharyan A et al April 2010 Risk of rehospitalization for patients using clopidogrel with a proton pump inhibitor PDF Arch Intern Med 170 8 704 10 doi 10 1001 archinternmed 2010 34 ISSN 1538 3679 PMID 20421557 Archived from the original on 4 March 2016 Wathion N Public statement on possible interaction between clopidogrel and proton pump inhibitors PDF Archived PDF from the original on 6 February 2011 Retrieved 31 March 2011 Hughes S EMEA issues warning on possible clopidogrel PPI interaction but is there really a problem Archived from the original on 22 May 2013 Retrieved 31 March 2011 Zakarija A Bandarenko N Pandey DK et al 2004 Clopidogrel Associated TTP An Update of Pharmacovigilance Efforts Conducted by Independent Researchers Pharmaceutical Suppliers and the Food and Drug Administration Stroke 35 2 533 8 doi 10 1161 01 STR 0000109253 66918 5E PMID 14707231 Diener HC Bogousslavsky J Brass LM et al 2004 Aspirin and clopidogrel compared with clopidogrel alone after recent ischaemic stroke or transient ischaemic attack in high risk patients MATCH randomised double blind placebo controlled trial The Lancet 364 9431 331 7 doi 10 1016 S0140 6736 04 16721 4 PMID 15276392 S2CID 9874277 a b Jasek W ed 2007 Austria Codex in German 62nd ed Vienna Osterreichischer Apothekerverlag pp 6526 7 ISBN 978 3 85200 181 4 DeNoon DJ 23 February 2016 FDA Warns Plavix Patients of Drug Interactions WebMD Archived from the original on 23 February 2016 Retrieved 23 November 2009 Public Health Advisory Updated Safety Information about a drug interaction between Clopidogrel Bisulfate marketed as Plavix and Omeprazole marketed as Prilosec and Prilosec OTC Food and Drug Administration FDA 17 November 2009 Archived from the original on 29 December 2009 Retrieved 13 March 2010 Farhat N Haddad N Crispo J et al February 2019 Trends in concomitant clopidogrel and proton pump inhibitor treatment among ACS inpatients 2000 2016 Eur J Clin Pharmacol 75 2 227 235 doi 10 1007 s00228 018 2564 8 PMID 30324301 S2CID 53085923 Wedemeyer RS Blume H 2014 Pharmacokinetic Drug Interaction Profiles of Proton Pump Inhibitors An Update Drug Safety 37 4 201 11 doi 10 1007 s40264 014 0144 0 PMC 3975086 PMID 24550106 John J Koshy SK 2012 Current Oral Antiplatelets Focus Update on Prasugrel The Journal of the American Board of Family Medicine 25 3 343 349 doi 10 3122 jabfm 2012 03 100270 PMID 22570398 a b c Cattaneo M March 2012 Response variability to clopidogrel is tailored treatment based on laboratory testing the right solution Journal of Thrombosis and Haemostasis 10 3 327 36 doi 10 1111 j 1538 7836 2011 04602 x PMID 22221409 S2CID 34477003 a b Pereillo JM Maftouh M Andrieu A et al 2002 Structure and stereochemistry of the active metabolite of clopidogrel Drug Metab Dispos 30 11 1288 95 doi 10 1124 dmd 30 11 1288 PMID 12386137 S2CID 2493588 Mega JL Close SL Wiviott SD et al January 2009 Cytochrome p 450 polymorphisms and response to clopidogrel The New England Journal of Medicine 360 4 354 62 doi 10 1056 NEJMoa0809171 PMID 19106084 Simon T Verstuyft C Mary Krause M et al January 2009 Genetic Determinants of Response to Clopidogrel and Cardiovascular Events The New England Journal of Medicine 360 4 363 75 doi 10 1056 NEJMoa0808227 PMID 19106083 Collet JP Hulot JS Pena A et al January 2009 Cytochrome P450 2C19 polymorphism in young patients treated with clopidogrel after myocardial infarction a cohort study The Lancet 373 9660 309 17 doi 10 1016 S0140 6736 08 61845 0 PMID 19108880 S2CID 22405890 a b Safety announcement Reduced effectiveness of Plavix in patients who are poor metabolizers U S Food and Drug Administration 3 August 2017 Archived from the original on 15 March 2010 FDA Drug Safety Communication Reduced effectiveness of Plavix clopidogrel in patients who are poor metabolizers of the drug U S Food and Drug Administration FDA 28 June 2019 Archived from the original on 18 June 2019 Retrieved 30 January 2022 Alkattan A Alsalameen E June 2021 Polymorphisms of genes related to phase I metabolic enzymes affecting the clinical efficacy and safety of clopidogrel treatment Expert Opinion on Drug Metabolism amp Toxicology 17 6 685 95 doi 10 1080 17425255 2021 1925249 PMID 33931001 S2CID 233470717 Clopidogrel Multum Consumer Information New products and markets fuel growth in 2005 IMS Health Archived from the original on 3 June 2008 Retrieved 2 March 2009 Top Ten Global Products 2007 PDF IMS Health 26 February 2008 Archived PDF from the original on 25 February 2011 Retrieved 2 March 2009 Details for Plavix Archived from the original on 14 August 2014 verification needed Topol EJ Schork NJ January 2011 Catapulting clopidogrel pharmacogenomics forward Nature Medicine 17 1 40 41 doi 10 1038 nm0111 40 PMID 21217678 S2CID 32083067 Preliminary Injunction Against Apotex Upheld on Appeal Press release Bristol Myers Squibb 8 December 2006 Archived from the original on 14 April 2014 Retrieved 14 March 2010 U S judge upholds Bristol Sanofi patent on Plavix Reuters 19 June 2007 Archived from the original on 20 May 2011 Retrieved 5 September 2007 FDA Gives Plavix a 6 Month Extension Patent Now Expires on 17 May 2012 26 January 2011 Archived from the original on 12 October 2011 Retrieved 12 January 2012 FDA approves generic versions of blood thinner Plavix Press release Food and Drug Administration FDA 17 May 2012 Archived from the original on 11 March 2016 Hogan DF Andrews DA Green HW et al 2004 Antiplatelet effects and pharmacodynamics of clopidogrel in cats J Am Vet Med Assoc 225 9 1406 1411 doi 10 2460 javma 2004 225 1406 PMID 15552317 Further reading EditDean L 2012 Clopidogrel Therapy and CYP2C19 Genotype In Pratt VM McLeod HL Rubinstein WS et al eds Medical Genetics Summaries National Center for Biotechnology Information NCBI PMID 28520346 Bookshelf ID NBK84114 External links Edit Clopidogrel Drug Information Portal U S National Library of Medicine US Patent US4847265A for Dextro rotatory enantiomer of methyl alpha 5 4 5 6 7 tetrahydro 3 2 c thieno pyridyl 2 chlorophenyl acetate and the pharmaceutical compositions containing it Portal nbsp Medicine Retrieved from https en wikipedia org w index php title Clopidogrel amp oldid 1170482177, wikipedia, wiki, book, books, library,

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