Pular para o conteúdo principal

Antihistamínicos

Profissionais de Saúde

Os artigos de Referência Profissional são projetados para uso por profissionais de saúde. Eles são escritos por médicos do Reino Unido e baseados em evidências de pesquisa, diretrizes do Reino Unido e da Europa. Você pode encontrar o Antihistamínicos artigo mais útil, ou um dos nossos outros artigos de saúde.

What are antihistamines?

This article focuses on antihistamines that antagonise histamine H1 receptors (histamine H1-receptor antagonists).

Other antihistamines - H2 antagonists, sometimes referred to as H2RAs or H2 blockers, block the action of histamine at the histamine H2 receptors of the parietal cells in the stomach. This decreases the production of stomach acid. H2 antagonists can be used in the treatment of dispepsia, peptic ulcers e doença do refluxo gastroesofágico.

Indicações1

They are used primarily to treat disorders where abnormal or excessive histamine release by inflammatory cells is thought to underly illness. This includes conditions such as:

  • Rinite - especially seasonal allergic rhinitis (hay fever).2

  • Urticária.

  • Anafilaxia (although evidence remains unclear).3

  • Angioedema.

  • Asma - antihistamines may have a minor role in asthma treatment, particularly if there is associated rhinitis.

Other conditions such as hyper-reactive (vasomotor) rhinitis e prurido of any cause are commonly treated with antihistamines, although there is little evidence that histamine plays a contributory role.

Other uses

  • Topically on the eye to treat allergic conjunctivitis, allergic rhinitis and on the skin for pruritus (eg, bites where they have limited efficacy and may cause sensitisation).

  • Nausea and vertigo - eg, cinnarizine, cyclizine.

  • Cough suppressants.

  • Terminal care for their sedating and anti-emetic effects.

  • Sometimes prescribed as sedatives for children (unlicensed, and not recommended).

Classificação

First- and second-generation antihistamines

First-generation 'sedating' antihistamines

Second-generation 'non-sedating' antihistamines

Alimemazine (formerly trimeprazine).

Chlorphenamine (formerly chlorpheniramine).

Clemastine.

Ciproheptadina.

Hydroxyzine.

Prometazina.

Acrivastina.

Cetirizina.

Desloratadine (a metabolite of loratadine).

Fexofenadina.

Levocetirizine (laevorotatory isomer of cetirizine).

Loratadina.

Mizolastine.

First-generation 'sedating' antihistamines

  • These are highly lipid-soluble, crossing the blood-brain barrier with ease and antagonise H1 receptors in both the CNS and periphery.

  • They cause sedation, cognitive impairment, motor retardation and, in certain individuals, agitation/stimulation.

  • These properties are sometimes useful for treating conditions where sleep is disturbed due to symptoms of urticaria or atopic dermatitis.

  • Alimemazine and promethazine are considered to be the most sedating, whilst chlorphenamine and cyclizine are considered to be the least so (of the 'sedating' group).4

  • They may also antagonise muscarinic acetylcholine receptors, causing symptoms such as dry mouth, urinary retention and confusion in the elderly.

Second-generation 'non-sedating' antihistamines

  • These are newer drugs.

  • Larger molecules and less lipophilic, and thus less likely to cross the blood-brain barrier.

  • However, all antihistamines can cross the blood-brain barrier to some degree and cause psychomotor impairment in susceptible individuals.5

  • Sedation - although some drugs are more sedating than others, the sedative tendency varies from patient to patient and so all patients must be warned of this and the potential danger. Alcohol increases any sedative effect and should be avoided. Drowsiness tends to diminish over time.

  • Paradoxical stimulation may also occur and this is a particular problem for some children. Use of a test dose prior to using the drug in a given situation is advisable to avoid this idiosyncratic reaction.

  • Arrhythmias - second-generation antihistamines mizolastine and terfenadine are particularly prone to cause ventricular arrhythmias (predominantly ventricular tachycardia and torsades de pointes).6 This is more likely to occur where a relatively high dose is being taken or where there is hepatic cytochrome P450 impairment, both of which raise the plasma concentration of the drug. Of the first-generation drugs, alimemazine, hydroxyzine and promethazine have been implicated as causing this complication. For this reason, terfenadine and astemizole have been withdrawn. Hypokalaemia or hypomagnesaemia increases the risk of this complication, as does pre-existing QT prolongation.

Important interactions1

  • Tricyclic antidepressants - antimuscarinic and sedative effects are potentially enhanced by co-administration of antihistamines.

  • Co-administration of antifungal imidazoles (eg, ketoconazole, itraconazole) and macrolide antibiotics (eg, erythromycin, clarithromycin) is to be avoided, as these drugs interact and raise the plasma concentration of second-generation antihistamines.

Choice of agents and evidence of effectiveness

Rinite alérgica

A comparative study suggests greater efficacy for levocetirizine compared to desloratadine. Cetirizine and levocetirizine have been shown to be beneficial in children.2 7 Long-term use of cetirizine by children with atopic dermatitis appears to have no impact on their behavioural, cognitive and psychomotor development.8

Chronic idiopathic urticaria

There is little evidence that antihistamines used symptomatically to treat nonspecific itching have any effect greater than placebo. Most of the second-generation antihistamines have been shown to benefit chronic idiopathic urticaria. Once-daily fexofenadine appears to offer effective and well-tolerated relief from the symptoms of this illness.9

Atualizações exclusivas para profissionais de saúde

Mantenha-se informado com as últimas atualizações clínicas, insights profissionais e orientações baseadas em evidências. O boletim informativo Patient Pro seleciona conteúdo essencial para profissionais de saúde—entregue diretamente na sua caixa de entrada.

Por favor, insira um endereço de e-mail válido

Ao se inscrever, você aceita nossos Política de Privacidade. Você pode cancelar a inscrição a qualquer momento. Nunca vendemos seus dados.

Leitura adicional e referências

  • Blaiss MS; Antihistamines: treatment selection criteria for pediatric seasonal allergic rhinitis. Allergy Asthma Proc. 2005 Mar-Apr;26(2):95-102.
  1. Formulário Nacional Britânico (BNF); Serviços de Evidências NICE (acesso apenas no Reino Unido)
  2. Mosges R, Konig V, Koberlein J; The effectiveness of modern antihistamines for treatment of allergic rhinitis - an IPD meta-analysis of 140,853 patients. Allergol Int. 2013 Jun;62(2):215-22. doi: 10.2332/allergolint.12-OA-0486. Epub 2013 Mar 25.
  3. Nurmatov UB, Rhatigan E, Simons FE, et al; H2-antihistamines for the treatment of anaphylaxis with and without shock: a systematic review. Ann Allergy Asthma Immunol. 2014 Feb;112(2):126-31. doi: 10.1016/j.anai.2013.11.010. Epub 2013 Dec 5.
  4. Ng KH, Chong D, Wong CK, et al; Central nervous system side effects of first- and second-generation antihistamines in school children with perennial allergic rhinitis: a randomized, double-blind, placebo-controlled comparative study. Pediatrics. 2004 Feb;113(2):e116-21.
  5. Ramaekers JG, Vermeeren A; All antihistamines cross blood-brain barrier. BMJ. 2000 Sep 2;321(7260):572.
  6. Recanatini M, Poluzzi E, Masetti M, et al; QT prolongation through hERG K(+) channel blockade: current knowledge and strategies for the early prediction during drug development. Med Res Rev. 2005 Mar;25(2):133-66.
  7. de Blic J, Wahn U, Billard E, et al; Levocetirizine in children: evidenced efficacy and safety in a 6-week randomized seasonal allergic rhinitis trial. Pediatr Allergy Immunol. 2005 May;16(3):267-75.
  8. Stevenson J, Cornah D, Evrard P, et al; Long-term evaluation of the impact of the h1-receptor antagonist cetirizine on the behavioral, cognitive, and psychomotor development of very young children with atopic dermatitis. Pediatr Res. 2002 Aug;52(2):251-7.
  9. Kaplan AP, Spector SL, Meeves S, et al; Once-daily fexofenadine treatment for chronic idiopathic urticaria: a multicenter, randomized, double-blind, placebo-controlled study. Ann Allergy Asthma Immunol. 2005 Jun;94(6):662-9.

Sobre o autorVer biografia completa

Imagem do autor

Dr Colin Tidy, MRCGP

Médico Generalista, Autor Médico

MBBS, MRCGP, MRCP (Paediatrics), DCH

Dr Colin Tidy é um médico do NHS, baseado em Oxfordshire.

Sobre o revisorVer biografia completa

Imagem do autor

Dr Krishna Vakharia, MRCGP

Diretor Médico de Saúde, Optum UK

MBChB, MRCGP(2013), BMedSci (hons), DFSRH, DRCOG, PGDipDerm (Distn)

Dr. Krishna Vakharia é uma médica de clínica geral do NHS. Ela também é examinadora regular do Diploma de Pós-Graduação em Dermatologia Prática na Universidade de Cardiff, além de ser a Diretora Médica de Saúde na Optum UK.

Histórico do artigo

As informações nesta página são escritas e revisadas por clínicos qualificados.

verificador de elegibilidade para gripe

Pergunte, compartilhe, conecte-se.

Navegue por discussões, faça perguntas e compartilhe experiências em centenas de tópicos de saúde.

verificador de sintomas

Sentindo-se mal?

Avalie seus sintomas online gratuitamente