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Wikipedia

Cetirizine

January 01, 1970

Cetirizine is a second-generation antihistamine used to treat allergic rhinitis (hay fever), dermatitis, and urticaria (hives).[5] It is taken by mouth.[6] Effects generally begin within thirty minutes and last for about a day.[6] The degree of benefit is similar to other antihistamines such as diphenhydramine, which is a first-generation antihistamine.[6]

Cetirizine
Clinical data
Pronunciation/sɛˈtɪrɪzn/
Trade namesAllacan, Piriteze, Zyrtec, others
AHFS/Drugs.comMonograph
MedlinePlusa698026
License data
Pregnancy
category
  • AU: B2
Routes of
administration		By mouth
ATC code
Legal status
Legal status
Pharmacokinetic data
BioavailabilityWell-absorbed (>70%)[1]
Protein binding88–96%[1]
MetabolismMinimal (non-cytochrome P450-mediated)[3][2]
Onset of action20–42 minutes[2]
Elimination half-lifeMean: 8.3 hours[3][2]
Range: 6.5–10 hours[4]
Duration of action≥24 hours[4]
ExcretionUrine: 70–85%[3]
Feces: 10–13%[3]
Identifiers
  • (±)-[2-[4-[(4-Chlorophenyl)phenylmethyl]-1-piperazinyl]ethoxy]acetic acid
CAS Number
  • 83881-51-0 Y
PubChem CID
  • 2678
IUPHAR/BPS
  • 1222
DrugBank
  • DB00341 Y
ChemSpider
  • 2577 Y
UNII
  • YO7261ME24
KEGG
  • D07662 Y
ChEBI
  • CHEBI:3561 Y
ChEMBL
  • ChEMBL1000 Y
CompTox Dashboard (EPA)
  • DTXSID4022787
ECHA InfoCard100.223.545
Chemical and physical data
FormulaC21H25ClN2O3
Molar mass388.89 g·mol−1
3D model (JSmol)
  • Interactive image
  • Clc1ccc(cc1)C(c2ccccc2)N3CCN(CC3)CCOCC(=O)O
  • InChI=1S/C21H25ClN2O3/c22-19-8-6-18(7-9-19)21(17-4-2-1-3-5-17)24-12-10-23(11-13-24)14-15-27-16-20(25)26/h1-9,21H,10-16H2,(H,25,26) Y
  • Key:ZKLPARSLTMPFCP-UHFFFAOYSA-N Y
  (verify)

Common side effects include sleepiness, dry mouth, headache, and abdominal pain.[6] The degree of sleepiness that occurs is generally less than with first-generation antihistamines because second-generation antihistamines are more selective for the H1 receptor.[7][5] Compared to other second-generation anti-histamines, cetirizine can cause drowsiness.[7] Second-generation antihistamines that do not cause drowsiness are fexofenadine, and loratadine.[7]

Use in pregnancy appears safe, but use during breastfeeding is not recommended.[8] The medication works by blocking histamine H1 receptors, mostly outside the brain.[6]

Cetirizine can be used for paediatric patients. The main side effect to be cautious about is somnolence.[9]

It was patented in 1983[10][11] and came into medical use in 1987.[12] It is on the World Health Organization's List of Essential Medicines.[13] It is available as a generic medication.[5] In 2021, it was the 49th most commonly prescribed medication in the United States, with more than 13 million prescriptions.[14][15]

Medical uses edit

Allergies edit

Cetirizine's primary indication is for hay fever and other allergies. Because the symptoms of itching and redness in these conditions are caused by histamine acting on the H1 receptor, blocking those receptors temporarily relieves those symptoms.[16]

Cetirizine is also commonly prescribed to treat acute and (in particular cases) chronic urticaria, more efficiently than any other second-generation antihistamine.[16]

Available forms edit

Cetirizine is available over-the-counter in the US in the form of 5 and 10 mg tablets. A 20 mg strength is available by prescription only.[3] It is also available as a 1 mg/mL syrup for oral administration by prescription. In the UK, up to 30 tablets of 10 mg are on the general sales list (of pharmaceuticals) and can be purchased without a prescription and without pharmacist supervision.[17] The drug can be in the form of tablets, capsules or a syrup.[17]

Adverse effects edit

Commonly reported side effects of cetirizine include headache, dry mouth, drowsiness, and fatigue, while more serious, but rare, adverse effects reported include tachycardia and edema.[18]

Pruritus after discontinuation of cetirizine edit

Discontinuing cetirizine after prolonged use (typically, use beyond six months) may result in pruritus (generalized itchiness).[19][20][21]

The United States Food and Drug Administration (FDA) analyzed cases of pruritus after stopping cetirizine in the FDA Adverse Event Reporting System (FAERS) database and medical literature through 24 April 2017. Their report noted that some patients indicated the itchiness impacted their ability to work, sleep or perform normal daily activities.[22]

No specific schedule for weaning is currently provided in the drug information for cetirizine.[23]

Pharmacology edit

 
L-Stereoisomer, levocetirizine (top) and D-stereoisomer of cetirizine.

Pharmacodynamics edit

Cetirizine acts as a highly selective antagonist of the histamine H1 receptor.[3] The Ki values for the H1 receptor are approximately 6 nM for cetirizine, 3 nM for levocetirizine, and 100 nM for dextrocetirizine, indicating that the levorotatory enantiomer is the main active form.[3] Cetirizine has 600-fold or greater selectivity for the H1 receptor over a wide variety of other sites, including muscarinic acetylcholine, serotonin, dopamine, and α-adrenergic receptors, among many others.[3] The drug shows 20,000-fold or greater selectivity for the H1 receptor over the five muscarinic acetylcholine receptors, and hence does not exhibit anticholinergic effects.[24][25] It shows negligible inhibition of the hERG channel (IC50Tooltip half-maximal inhibitory concentration > 30 μM)[26] and no cardiotoxicity has been observed with cetirizine at doses of up to 60 mg/day, six times the normal recommended dose[3] and the highest dose of cetirizine that has been studied in healthy subjects.[27]

Cetirizine crosses the blood–brain barrier only slightly, and for this reason, produces minimal sedation compared to many other antihistamines.[28] A positron emission tomography (PET) study found that brain occupancy of the H1 receptor was 12.6% for 10 mg cetirizine, 25.2% for 20 mg cetirizine, and 67.6% for 30 mg hydroxyzine.[29] (A 10 mg dose of cetirizine equals about a 30 mg dose of hydroxyzine in terms of peripheral antihistamine effect.)[30] PET studies with antihistamines have found that brain H1 receptor occupancy of more than 50% is associated with a high prevalence of somnolence and cognitive decline, whereas brain H1 receptor occupancy of less than 20% is considered to be non-sedative.[31] In accordance, H1 receptor occupancy correlated well with subjective sleepiness for 30 mg hydroxyzine but there was no correlation for 10 or 20 mg cetirizine.[29] As such, brain penetration and brain H1 receptor occupancy by cetirizine are dose-dependent, and in accordance, while cetirizine at doses of 5 to 10 mg have been reported to be non-sedating or mildly sedating, a higher dose of 20 mg has been found to induce significant drowsiness in other studies.[29]

Cetirizine also shows anti-inflammatory properties independent of H1 receptors.[32] The effect is exhibited through suppression of the NF-κB pathway, and by regulating the release of cytokines and chemokines, thereby regulating the recruitment of inflammatory cells.[33][34][35][36][37] It has been shown to inhibit eosinophil chemotaxis and LTB4 release.[38] At a dosage of 20 mg, Boone et al. found that it inhibited the expression of VCAM-1 in patients with atopic dermatitis.[38]

Pharmacokinetics edit

Absorption edit

Cetirizine is rapidly and extensively absorbed upon oral administration in tablet or syrup form.[3] The oral bioavailability of cetirizine is at least 70% and of levocetirizine is at least 85%.[1] The Tmax of cetirizine is approximately 1.0 hour regardless of formulation.[2] The pharmacokinetics of cetirizine have been found to increase linearly with dose across a range of 5 to 60 mg.[3] Its Cmax following a single dose has been found to be 257 ng/mL for 10 mg and 580 ng/mL for 20 mg.[2] Food has no effect on the bioavailability of cetirizine but has been found to delay the Tmax by 1.7 hours (i.e., to approximately 2.7 hours) and to decrease the Cmax by 23%.[3][2][39] Similar findings were reported for levocetirizine, which had its Tmax delayed by 1.25 hours and its Cmax decreased by about 36% when administered with a high-fat meal.[39] Steady-state levels of cetirizine occur within 3 days and there is no accumulation of the drug with chronic administration.[2] Following once-daily administration of 10 mg cetirizine for ten days, the mean Cmax was 311 ng/mL.[40]

Distribution edit

The mean plasma protein binding of cetirizine has been found to be 93 to 96% across a range of 25 to 1,000 ng/mL independent of concentration.[2] Plasma protein binding of 88 to 96% has also been reported across multiple studies.[1] The drug is bound to albumin with high affinity, while α1-acid glycoprotein and lipoproteins contribute much less to total plasma protein binding.[1] The unbound or free fraction of levocetirizine has been reported to be 8%.[1] The true volume of distribution of cetirizine is unknown but is estimated to be 0.3 to 0.45 L/kg.[3][1] Cetirizine poorly and slowly crosses the blood–brain barrier, which is thought to be due to its chemical properties and its activity as a P-glycoprotein substrate.[41][1][42]

Metabolism edit

Cetirizine does not undergo extensive metabolism.[3] It is notably not metabolized by the cytochrome P450 system.[43] Because of this, it does not interact significantly with drugs that inhibit or induce cytochrome P450 enzymes such as theophylline, erythromycin, clarithromycin, cimetidine, or alcohol.[3] While cetirizine does not undergo extensive metabolism or metabolism by the cytochrome P450 enzyme, it does undergo some metabolism by other means, the metabolic pathways of which include oxidation and conjugation.[3][2] Plasma radioactivity attributed to unchanged cetirizine is more than 90% at 2 hours, 80% at 10 hours, and 70% at 24 hours, indicating limited and slow metabolism.[2] The enzymes responsible for transformation of cetirizine have not been identified.[3]

Elimination edit

Cetirizine is eliminated approximately 70 to 85% in the urine and 10 to 13% in the feces.[3] About 50 or 60% of cetirizine eliminated in the urine is unchanged.[3][2] It is eliminated in the urine via an active transport mechanism.[2] The elimination half-life of cetirizine ranges from 6.5 to 10 hours in healthy adults, with a mean across studies of approximately 8.3 hours.[3][2] Its duration of action is at least 24 hours.[2] The elimination half-life of cetirizine is increased in the elderly (to 12 hours), in hepatic impairment (to 14 hours), and in renal impairment (to 20 hours).[2]

Chemistry edit

Cetirizine contains L- and D-stereoisomers. Chemically, levocetirizine is the active L-enantiomer of cetirizine. The drug is a member of the diphenylmethylpiperazine group of antihistamines. Analogues include cyclizine and hydroxyzine.[44]

Synthesis edit

 
Cetirizine synthesis:[10]

The 1-(4-chlorophenylmethyl)-piperazine is alkylated with methyl (2-chloroethoxy)-acetate in the presence of sodium carbonate and xylene solvent to produce the Sn2 substitution product in 28% yield. Saponification of the acetate ester is done by refluxing with potassium hydroxide in absolute ethanol to afford a 56% yield of the potassium salt intermediate. This is then hydrolyzed with aqueous HCl and extracted to give an 81% yield of the carboxylic acid product.[45]

Availability edit

 
A package of 10 mg cetirizine tablets.
 
Zyrtec-D, a combination of cetirizine and pseudoephedrine.

Cetirizine is available without a prescription.[46] In some countries it is available over-the-counter only in packages containing seven or ten 10 mg doses.[47][48]

Cetirizine is available as a combination medication with pseudoephedrine, a decongestant.[49] The combination is often marketed using the same brand name as the cetirizine with a "-D" suffix (for example, Zyrtec-D).[50][51]

Cetirizine is marketed under the brand names Alatrol, Alerid, Allacan, Allercet, Alzene, Cerchio, Cetirin, Cetizin, Cetriz, Cetzine, Cezin, Cetgel, Cirrus, Histec, Histazine, Humex, Letizen, Okacet (Cipla), Piriteze, Reactine, Razene, Rigix, Sensahist (Oethmann, South Africa), Triz, Zetop, Zirtec, Zirtek, Zodac, Zyllergy, Zynor, Zyrlek, and Zyrtec (Johnson & Johnson), inter alios.[52][53][failed verification]

References edit

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January 01, 1970
cetirizine, second, generation, antihistamine, used, treat, allergic, rhinitis, fever, dermatitis, urticaria, hives, taken, mouth, effects, generally, begin, within, thirty, minutes, last, about, degree, benefit, similar, other, antihistamines, such, diphenhyd. Cetirizine is a second generation antihistamine used to treat allergic rhinitis hay fever dermatitis and urticaria hives 5 It is taken by mouth 6 Effects generally begin within thirty minutes and last for about a day 6 The degree of benefit is similar to other antihistamines such as diphenhydramine which is a first generation antihistamine 6 CetirizineClinical dataPronunciation s ɛ ˈ t ɪr ɪ z iː n Trade namesAllacan Piriteze Zyrtec othersAHFS Drugs comMonographMedlinePlusa698026License dataUS DailyMed CetirizinePregnancycategoryAU B2Routes ofadministrationBy mouthATC codeR06AE07 WHO S01GX12 WHO Legal statusLegal statusAU Unscheduled CA OTC NZ OTC UK General sales list GSL OTC P US OTC Rx only OTC Rx onlyPharmacokinetic dataBioavailabilityWell absorbed gt 70 1 Protein binding88 96 1 MetabolismMinimal non cytochrome P450 mediated 3 2 Onset of action20 42 minutes 2 Elimination half lifeMean 8 3 hours 3 2 Range 6 5 10 hours 4 Duration of action 24 hours 4 ExcretionUrine 70 85 3 Feces 10 13 3 IdentifiersIUPAC name 2 4 4 Chlorophenyl phenylmethyl 1 piperazinyl ethoxy acetic acidCAS Number83881 51 0 YPubChem CID2678IUPHAR BPS1222DrugBankDB00341 YChemSpider2577 YUNIIYO7261ME24KEGGD07662 YChEBICHEBI 3561 YChEMBLChEMBL1000 YCompTox Dashboard EPA DTXSID4022787ECHA InfoCard100 223 545Chemical and physical dataFormulaC 21H 25Cl N 2O 3Molar mass388 89 g mol 13D model JSmol Interactive imageSMILES Clc1ccc cc1 C c2ccccc2 N3CCN CC3 CCOCC O OInChI InChI 1S C21H25ClN2O3 c22 19 8 6 18 7 9 19 21 17 4 2 1 3 5 17 24 12 10 23 11 13 24 14 15 27 16 20 25 26 h1 9 21H 10 16H2 H 25 26 YKey ZKLPARSLTMPFCP UHFFFAOYSA N Y verify Common side effects include sleepiness dry mouth headache and abdominal pain 6 The degree of sleepiness that occurs is generally less than with first generation antihistamines because second generation antihistamines are more selective for the H1 receptor 7 5 Compared to other second generation anti histamines cetirizine can cause drowsiness 7 Second generation antihistamines that do not cause drowsiness are fexofenadine and loratadine 7 Use in pregnancy appears safe but use during breastfeeding is not recommended 8 The medication works by blocking histamine H1 receptors mostly outside the brain 6 Cetirizine can be used for paediatric patients The main side effect to be cautious about is somnolence 9 It was patented in 1983 10 11 and came into medical use in 1987 12 It is on the World Health Organization s List of Essential Medicines 13 It is available as a generic medication 5 In 2021 it was the 49th most commonly prescribed medication in the United States with more than 13 million prescriptions 14 15 Contents 1 Medical uses 1 1 Allergies 1 2 Available forms 2 Adverse effects 2 1 Pruritus after discontinuation of cetirizine 3 Pharmacology 3 1 Pharmacodynamics 3 2 Pharmacokinetics 3 2 1 Absorption 3 2 2 Distribution 3 2 3 Metabolism 3 2 4 Elimination 4 Chemistry 4 1 Synthesis 5 Availability 6 ReferencesMedical uses editAllergies edit Cetirizine s primary indication is for hay fever and other allergies Because the symptoms of itching and redness in these conditions are caused by histamine acting on the H1 receptor blocking those receptors temporarily relieves those symptoms 16 Cetirizine is also commonly prescribed to treat acute and in particular cases chronic urticaria more efficiently than any other second generation antihistamine 16 Available forms edit Cetirizine is available over the counter in the US in the form of 5 and 10 mg tablets A 20 mg strength is available by prescription only 3 It is also available as a 1 mg mL syrup for oral administration by prescription In the UK up to 30 tablets of 10 mg are on the general sales list of pharmaceuticals and can be purchased without a prescription and without pharmacist supervision 17 The drug can be in the form of tablets capsules or a syrup 17 Adverse effects editCommonly reported side effects of cetirizine include headache dry mouth drowsiness and fatigue while more serious but rare adverse effects reported include tachycardia and edema 18 Pruritus after discontinuation of cetirizine edit Discontinuing cetirizine after prolonged use typically use beyond six months may result in pruritus generalized itchiness 19 20 21 The United States Food and Drug Administration FDA analyzed cases of pruritus after stopping cetirizine in the FDA Adverse Event Reporting System FAERS database and medical literature through 24 April 2017 Their report noted that some patients indicated the itchiness impacted their ability to work sleep or perform normal daily activities 22 No specific schedule for weaning is currently provided in the drug information for cetirizine 23 Pharmacology edit nbsp L Stereoisomer levocetirizine top and D stereoisomer of cetirizine Pharmacodynamics edit Cetirizine acts as a highly selective antagonist of the histamine H1 receptor 3 The Ki values for the H1 receptor are approximately 6 nM for cetirizine 3 nM for levocetirizine and 100 nM for dextrocetirizine indicating that the levorotatory enantiomer is the main active form 3 Cetirizine has 600 fold or greater selectivity for the H1 receptor over a wide variety of other sites including muscarinic acetylcholine serotonin dopamine and a adrenergic receptors among many others 3 The drug shows 20 000 fold or greater selectivity for the H1 receptor over the five muscarinic acetylcholine receptors and hence does not exhibit anticholinergic effects 24 25 It shows negligible inhibition of the hERG channel IC50Tooltip half maximal inhibitory concentration gt 30 mM 26 and no cardiotoxicity has been observed with cetirizine at doses of up to 60 mg day six times the normal recommended dose 3 and the highest dose of cetirizine that has been studied in healthy subjects 27 Cetirizine crosses the blood brain barrier only slightly and for this reason produces minimal sedation compared to many other antihistamines 28 A positron emission tomography PET study found that brain occupancy of the H1 receptor was 12 6 for 10 mg cetirizine 25 2 for 20 mg cetirizine and 67 6 for 30 mg hydroxyzine 29 A 10 mg dose of cetirizine equals about a 30 mg dose of hydroxyzine in terms of peripheral antihistamine effect 30 PET studies with antihistamines have found that brain H1 receptor occupancy of more than 50 is associated with a high prevalence of somnolence and cognitive decline whereas brain H1 receptor occupancy of less than 20 is considered to be non sedative 31 In accordance H1 receptor occupancy correlated well with subjective sleepiness for 30 mg hydroxyzine but there was no correlation for 10 or 20 mg cetirizine 29 As such brain penetration and brain H1 receptor occupancy by cetirizine are dose dependent and in accordance while cetirizine at doses of 5 to 10 mg have been reported to be non sedating or mildly sedating a higher dose of 20 mg has been found to induce significant drowsiness in other studies 29 Cetirizine also shows anti inflammatory properties independent of H1 receptors 32 The effect is exhibited through suppression of the NF kB pathway and by regulating the release of cytokines and chemokines thereby regulating the recruitment of inflammatory cells 33 34 35 36 37 It has been shown to inhibit eosinophil chemotaxis and LTB4 release 38 At a dosage of 20 mg Boone et al found that it inhibited the expression of VCAM 1 in patients with atopic dermatitis 38 Pharmacokinetics edit Absorption edit Cetirizine is rapidly and extensively absorbed upon oral administration in tablet or syrup form 3 The oral bioavailability of cetirizine is at least 70 and of levocetirizine is at least 85 1 The Tmax of cetirizine is approximately 1 0 hour regardless of formulation 2 The pharmacokinetics of cetirizine have been found to increase linearly with dose across a range of 5 to 60 mg 3 Its Cmax following a single dose has been found to be 257 ng mL for 10 mg and 580 ng mL for 20 mg 2 Food has no effect on the bioavailability of cetirizine but has been found to delay the Tmax by 1 7 hours i e to approximately 2 7 hours and to decrease the Cmax by 23 3 2 39 Similar findings were reported for levocetirizine which had its Tmax delayed by 1 25 hours and its Cmax decreased by about 36 when administered with a high fat meal 39 Steady state levels of cetirizine occur within 3 days and there is no accumulation of the drug with chronic administration 2 Following once daily administration of 10 mg cetirizine for ten days the mean Cmax was 311 ng mL 40 Distribution edit The mean plasma protein binding of cetirizine has been found to be 93 to 96 across a range of 25 to 1 000 ng mL independent of concentration 2 Plasma protein binding of 88 to 96 has also been reported across multiple studies 1 The drug is bound to albumin with high affinity while a1 acid glycoprotein and lipoproteins contribute much less to total plasma protein binding 1 The unbound or free fraction of levocetirizine has been reported to be 8 1 The true volume of distribution of cetirizine is unknown but is estimated to be 0 3 to 0 45 L kg 3 1 Cetirizine poorly and slowly crosses the blood brain barrier which is thought to be due to its chemical properties and its activity as a P glycoprotein substrate 41 1 42 Metabolism edit Cetirizine does not undergo extensive metabolism 3 It is notably not metabolized by the cytochrome P450 system 43 Because of this it does not interact significantly with drugs that inhibit or induce cytochrome P450 enzymes such as theophylline erythromycin clarithromycin cimetidine or alcohol 3 While cetirizine does not undergo extensive metabolism or metabolism by the cytochrome P450 enzyme it does undergo some metabolism by other means the metabolic pathways of which include oxidation and conjugation 3 2 Plasma radioactivity attributed to unchanged cetirizine is more than 90 at 2 hours 80 at 10 hours and 70 at 24 hours indicating limited and slow metabolism 2 The enzymes responsible for transformation of cetirizine have not been identified 3 Elimination edit Cetirizine is eliminated approximately 70 to 85 in the urine and 10 to 13 in the feces 3 About 50 or 60 of cetirizine eliminated in the urine is unchanged 3 2 It is eliminated in the urine via an active transport mechanism 2 The elimination half life of cetirizine ranges from 6 5 to 10 hours in healthy adults with a mean across studies of approximately 8 3 hours 3 2 Its duration of action is at least 24 hours 2 The elimination half life of cetirizine is increased in the elderly to 12 hours in hepatic impairment to 14 hours and in renal impairment to 20 hours 2 Chemistry editCetirizine contains L and D stereoisomers Chemically levocetirizine is the active L enantiomer of cetirizine The drug is a member of the diphenylmethylpiperazine group of antihistamines Analogues include cyclizine and hydroxyzine 44 Synthesis edit nbsp Cetirizine synthesis 10 The 1 4 chlorophenylmethyl piperazine is alkylated with methyl 2 chloroethoxy acetate in the presence of sodium carbonate and xylene solvent to produce the Sn2 substitution product in 28 yield Saponification of the acetate ester is done by refluxing with potassium hydroxide in absolute ethanol to afford a 56 yield of the potassium salt intermediate This is then hydrolyzed with aqueous HCl and extracted to give an 81 yield of the carboxylic acid product 45 Availability edit nbsp A package of 10 mg cetirizine tablets nbsp Zyrtec D a combination of cetirizine and pseudoephedrine Cetirizine is available without a prescription 46 In some countries it is available over the counter only in packages containing seven or ten 10 mg doses 47 48 Cetirizine is available as a combination medication with pseudoephedrine a decongestant 49 The combination is often marketed using the same brand name as the cetirizine with a D suffix for example Zyrtec D 50 51 Cetirizine is marketed under the brand names Alatrol Alerid Allacan Allercet Alzene Cerchio Cetirin Cetizin Cetriz Cetzine Cezin Cetgel Cirrus Histec Histazine Humex Letizen Okacet Cipla Piriteze Reactine Razene Rigix Sensahist Oethmann South Africa Triz Zetop Zirtec Zirtek Zodac Zyllergy Zynor Zyrlek and Zyrtec Johnson amp Johnson inter alios 52 53 failed verification References edit a b c d e f g h Chen C 2008 Physicochemical pharmacological and pharmacokinetic properties of the zwitterionic antihistamines cetirizine and levocetirizine Current Medicinal Chemistry 15 21 2173 2191 doi 10 2174 092986708785747625 PMID 18781943 a b c d e f g h i j k l m n o Simons FE Simons KJ May 1999 Clinical pharmacology of new histamine H1 receptor antagonists Clinical Pharmacokinetics 36 5 329 352 doi 10 2165 00003088 199936050 00003 PMID 10384858 S2CID 21360079 a b c d e f g h i j k l m n o p q r s t Portnoy JM Dinakar C January 2004 Review of cetirizine hydrochloride for the treatment of allergic disorders Expert Opinion on Pharmacotherapy 5 1 125 135 doi 10 1517 14656566 5 1 125 PMID 14680442 S2CID 28946859 a b Simons FE December 2002 Comparative pharmacology of H1 antihistamines clinical relevance The American Journal of Medicine 113 Suppl 9A 38S 46S doi 10 1016 s0002 9343 02 01436 5 PMID 12517581 a b c British national formulary BNF 76 76 ed Pharmaceutical Press 2018 p 279 ISBN 9780857113382 a b c d e Cetirizine Hydrochloride Monograph for Professionals Drugs com American Society of Health System Pharmacists Archived from the original on 28 August 2021 Retrieved 3 March 2019 a b c Slater JW Zechnich AD Haxby DG January 1999 Second generation antihistamines a comparative review Drugs 57 1 31 47 doi 10 2165 00003495 199957010 00004 PMID 9951950 S2CID 46984477 Cetirizine Pregnancy and Breastfeeding Warnings Drugs com Archived from the original on 6 March 2019 Retrieved 3 March 2019 Zhou P Jia Q Wang Z Zhao R Zhou W 25 August 2022 Cetirizine for the treatment of allergic diseases in children A systematic review and meta analysis Frontiers in Pediatrics 10 940213 doi 10 3389 fped 2022 940213 PMC 9452751 PMID 36090559 a b US patent 4525358 Baltes E De Lannoy J Rodriguez L 2 4 Diphenylmethyl 1 piperazinyl acetic acids and their amides issued 25 June 1985 assigned to UCB Pharmaceuticals Inc US4525358A Baltes Eugene Lannoy Jean de amp Rodriguez Ludovic 2 4 Diphenylmethyl 1 piperazinyl acetic acids and their amides issued 1985 06 25 Fischer J Ganellin CR 2006 Analogue based Drug Discovery John Wiley amp Sons p 549 ISBN 9783527607495 Archived from the original on 8 October 2022 Retrieved 19 September 2020 World Health Organization 2021 World Health Organization model list of essential medicines 22nd list 2021 Geneva World Health Organization hdl 10665 345533 WHO MHP HPS EML 2021 02 The Top 300 of 2021 ClinCalc Archived from the original on 15 January 2024 Retrieved 14 January 2024 Cetirizine Drug Usage Statistics ClinCalc Retrieved 14 January 2024 a b Rang HP Dale MM Flower RJ Henderson G 21 January 2015 Rang and Dale s pharmacology Eighth ed United Kingdom p 332 ISBN 978 0 7020 5362 7 OCLC 903083639 a href Template Cite book html title Template Cite book cite book a CS1 maint location missing publisher link a b CETIRIZINE HYDROCHLORIDE Archived from the original on 10 October 2022 Retrieved 17 October 2020 Zyrtec Side Effects drugs com Archived from the original on 23 July 2019 Retrieved 21 August 2015 Ekhart C van der Horst P van Hunsel F December 2016 Unbearable Pruritus After Withdrawal of Levo cetirizine Drug Safety Case Reports 3 1 16 doi 10 1007 s40800 016 0041 9 PMC 5124431 PMID 27889900 Cetirizine Zyrtec Withdrawal amp Unbearable Itching People s Pharmacy Archived from the original on 14 August 2013 Retrieved 9 September 2017 addicted to zyrtec MedHelp Archived from the original on 16 September 2017 Retrieved 9 September 2017 Chung AH La Grenade L Harinstein LM 2019 Pruritus after discontinuation of cetirizine Therapeutic Advances in Drug Safety 10 2042098619859996 doi 10 1177 2042098619859996 PMC 6613055 PMID 31308927 Borst H 18 May 2023 Did you know stopping Zyrtec can cause withdrawal The Checkup Retrieved 23 July 2023 Zhang L Cheng L Hong J 2013 The clinical use of cetirizine in the treatment of allergic rhinitis Pharmacology 92 1 2 14 25 doi 10 1159 000351843 PMID 23867423 Orzechowski RF Currie DS Valancius CA January 2005 Comparative anticholinergic activities of 10 histamine H1 receptor antagonists in two functional models European Journal of Pharmacology 506 3 257 264 doi 10 1016 j ejphar 2004 11 006 PMID 15627436 Taglialatela M Pannaccione A Castaldo P Giorgio G Zhou Z January CT et al July 1998 Molecular basis for the lack of HERG K channel block related cardiotoxicity by the H1 receptor blocker cetirizine compared with other second generation antihistamines Molecular Pharmacology 54 1 113 121 doi 10 1124 mol 54 1 113 PMID 9658196 Hulhoven R Rosillon D Letiexhe M Meeus MA Daoust A Stockis A November 2007 Levocetirizine does not prolong the QT QTc interval in healthy subjects results from a thorough QT study European Journal of Clinical Pharmacology 63 11 1011 1017 doi 10 1007 s00228 007 0366 5 PMID 17891537 S2CID 36218027 The equivalent dose of 60 mg cetirizine is also the highest dose ever administered in healthy subjects 13 Gupta A Chatelain P Massingham R Jonsson EN Hammarlund Udenaes M February 2006 Brain distribution of cetirizine enantiomers comparison of three different tissue to plasma partition coefficients K p K p u and K p uu Drug Metabolism and Disposition 34 2 318 323 doi 10 1124 dmd 105 007211 PMID 16303872 S2CID 9111905 a b c Tashiro M Kato M Miyake M Watanuki S Funaki Y Ishikawa Y et al October 2009 Dose dependency of brain histamine H 1 receptor occupancy following oral administration of cetirizine hydrochloride measured using PET with 11C doxepin Human Psychopharmacology 24 7 540 548 doi 10 1002 hup 1051 PMID 19697300 S2CID 5596000 van den Elzen MT van Os Medendorp H van den Brink I van den Hurk K Kouznetsova OI Lokin AS et al 2017 Effectiveness and safety of antihistamines up to fourfold or higher in treatment of chronic spontaneous urticaria Clinical and Translational Allergy 7 4 doi 10 1186 s13601 017 0141 3 PMC 5309999 PMID 28289538 30 mg of hydroxyzine equals about 10 mg cetirizine 11 Yanai K Tashiro M January 2007 The physiological and pathophysiological roles of neuronal histamine an insight from human positron emission tomography studies Pharmacology amp Therapeutics 113 1 1 15 doi 10 1016 j pharmthera 2006 06 008 PMID 16890992 Koller M Hilger RA Rihoux JP Konig W May 1996 Cetirizine exerts anti inflammatory effects on human neutrophils International Archives of Allergy and Immunology 110 1 52 56 doi 10 1159 000237310 PMID 8645978 Bielory L Lien KW Bigelsen S 2005 Efficacy and tolerability of newer antihistamines in the treatment of allergic conjunctivitis Drugs 65 2 215 228 doi 10 2165 00003495 200565020 00004 PMID 15631542 S2CID 46791611 Walsh GM January 1994 The anti inflammatory effects of cetirizine Clinical and Experimental Allergy 24 1 81 85 doi 10 1111 j 1365 2222 1994 tb00921 x PMID 8156449 S2CID 32269456 Gelfand EW Appajosyula S Meeves S January 2004 Anti inflammatory activity of H1 receptor antagonists review of recent experimental research Current Medical Research and Opinion 20 1 73 81 doi 10 1185 030079903125002586 PMID 14741075 S2CID 20451677 Fumagalli F Baiardini I Pasquali M Compalati E Guerra L Massacane P Canonica GW August 2004 Antihistamines do they work Further well controlled trials involving larger samples are needed Allergy 59 Suppl 78 74 77 doi 10 1111 j 1398 9995 2004 00573 x PMID 15245363 S2CID 39936983 Grob JJ Castelain M Richard MA Bonniol JP Beraud V Adhoute H et al May 1998 Antiinflammatory properties of cetirizine in a human contact dermatitis model Clinical evaluation of patch tests is not hampered by antihistamines Acta Dermato Venereologica 78 3 194 197 doi 10 1080 000155598441512 PMID 9602225 a b Boone M Lespagnard L Renard N Song M Rihoux JP July 2000 Adhesion molecule profiles in atopic dermatitis vs allergic contact dermatitis pharmacological modulation by cetirizine Journal of the European Academy of Dermatology and Venereology 14 4 263 266 doi 10 1046 j 1468 3083 2000 00017 x PMID 11204513 S2CID 24026684 a b Pasko P Rodacki T Domagala Rodacka R Palimonka K Marcinkowska M Owczarek D September 2017 Second generation H1 antihistamines interaction with food and alcohol A systematic review Biomedicine amp Pharmacotherapy 93 27 39 doi 10 1016 j biopha 2017 06 008 PMID 28622592 Zyrtec prescribing information PDF May 2006 Archived from the original PDF on 4 January 2010 Retrieved 19 November 2009 Hu Y Sieck DE Hsu WH October 2015 Why are second generation H1 antihistamines minimally sedating European Journal of Pharmacology 765 100 106 doi 10 1016 j ejphar 2015 08 016 PMID 26291661 Conen S Theunissen EL Vermeeren A van Ruitenbeek P Stiers P Mehta MA et al September 2013 The role of P glycoprotein in CNS antihistamine effects Psychopharmacology 229 1 9 19 doi 10 1007 s00213 013 3075 z PMID 23564211 S2CID 10416220 Mahmoudi M 2 June 2016 Allergy and Asthma Practical Diagnosis and Management Springer pp 574 ISBN 978 3 319 30835 7 Cetirizine PubChem U S Naionatl Library of Medicine Retrieved 4 April 2022 Reiter J Trinka P Bartha FL Pongo L Volk B Simig G 20 July 2012 New Manufacturing Procedure of Cetirizine Organic Process Research amp Development 16 7 1279 1282 doi 10 1021 op300009y ISSN 1083 6160 Cetirizine Clinical Review U S Food and Drug Administration 11 September 2016 Aaronson DW May 1996 Evaluation of cetirizine in patients with allergic rhinitis and perennial asthma Annals of Allergy Asthma amp Immunology 76 5 440 446 doi 10 1016 s1081 1206 10 63461 8 PMID 8630718 Jobst S van den Wijngaart W Schubert A van de Venne H September 1994 Assessment of the efficacy and safety of three dose levels of cetirizine given once daily in children with perennial allergic rhinitis Allergy 49 8 598 604 doi 10 1111 j 1398 9995 1994 tb00125 x PMID 7653736 S2CID 46312788 Wellington K Jarvis B 2001 Cetirizine pseudoephedrine Drugs 61 15 2231 2240 doi 10 2165 00003495 200161150 00009 PMID 11772135 S2CID 263997602 Nathan RA Finn AF LaForce C Ratner P Chapman D de Guia EC et al September 2006 Comparison of cetirizine pseudoephedrine and placebo in patients with seasonal allergic rhinitis and concomitant mild to moderate asthma randomized double blind study Annals of Allergy Asthma amp Immunology 97 3 389 396 doi 10 1016 S1081 1206 10 60806 X PMID 17042147 Antihistamine Decongestant Combination Oral Route Description and Brand Names Mayo Clinic 7 February 2023 Retrieved 23 February 2023 Cetirizine antihistamine that relieves allergy symptoms nhs uk 30 October 2018 Retrieved 23 October 2023 Protriptyline AHFS Patient Medication Information Internet Bethesda MD American Society of Health System Pharmacists Inc 2019 via Medlineplus Portal nbsp Medicine Retrieved from https en wikipedia org w index php title Cetirizine amp oldid 1218399995, wikipedia, wiki, book, books, 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