Urticaria is a common pediatric skin disorder. Histamine H1-receptor antagonists are effective in chronic as well as acute urticaria. When H1-anti-histamines are ineffective, add-on use of H2-receptor antagonists is thought to give better symptom relief. However, there are few reports on the therapeutic efficacy in pediatric patients. We retrospectively reviewed the medical records of pediatric patients with chronic spontaneous urticaria (csU) who met the following criteria. They were consulted our outpatient clinic between April 2010 and March 2012; were unsuccessfully treated with H1 antihistamines; and were treated with add-on H2-receptor antagonist (famotidine). In six patients who met the inclusion criteria (mean age 6.1 ± 5.1 years), urticaria activity score was significantly decreased from 4.3 ± 0.8 just before administration of famotidine to 1.3 ± 1.0 on the first outpatient visit within 4 weeks after the first administration of famotidine (p < 0.0001). No adverse effects of famotidine were observed. Although this study has a limitation of small subjects, our results suggest the potential efficacy of add-on use of H2-receptor antagonists and might justify extending the range of application of H2-receptor antagonists to pediatric patients with csU.
Urticaria is a fairly common skin disorder in children and is characterized by transient, pruritic, variably sized wheals with well-defined borders and central pallor. When urticaria occurs without any trigger, it is classified as spontaneous. In childhood, stimuli such as infection, foods, and medication easily provoke acute urticaria [
Recent guidelines recommend H1-receptor antagonists as first-line treatment for chronic as well as acute urticaria [7,8]. In cases where these fail to benefit csU, several step-up management options are suggested, including histamine H2-receptor antagonists, leukotriene-receptor antagonists (LTRA), ciclosporin, dapsone, and anti-immunoglobin E (IgE; omalizumab). Although a recent Cochrane Review could not resolve uncertainty over the role of H2-receptor antagonists in urticaria [
Regarding recent reviews on pediatric chronic urticaria, one put H2-receptor antagonists collectively in the same category with firstand second-generation H1- receptor antagonists as anti-histamines [
We report here a retrospective series of six pediatric patients with csU resistant to H1-receptor antagonists who were successfully treated with the H2-receptor antagonist, famotidine, in the past two years.
We retrospectively reviewed the medical records of pediatric patients who met the following criteria. They were diagnosed with csU according to the guideline [7,8]; consulted our outpatient clinic between April 2010 and March 2012; were unsuccessfully treated with H1 antihistamines including an alternative H1 agent and/or dose escalation of the original agent; and were treated with add-on famotidine.
In the acute management of urticaria, H1-receptor antagonists irrespective of the generations should be used. Famotidine (Gaster®, Astellas Pharma Inc., Tokyo) was chosen as H2-receptor antagonist for pediatric use as it has the advantage of being a powder formulation so that it can easily be taken by pediatric patients orally and the dose readily adjusted for the patient’s weight. H1- receptor antagonist treatment was continued at the start of famotidine administration. Famotidine was administered orally to each patient twice daily (1 mg/kg/day).
After famotidine treatment was commenced, patients consulted our outpatient clinic at a maximum of 4-week intervals. Therapeutic efficacy was evaluated using the urticaria activity score (UAS) [8,13].
Data are presented as mean ± SD. The significance of differences between two groups was determined by Student’s t test, with the level of significance set at p < 0.05. Analyses were performed using the GraphPad Prism (GraphPad Software, San Diego, CA).
Six patients (three male, three female) met the inclusion criteria.
Pre: Just before administration of famotidine; Post: On the first outpatient visit within 2 - 4 weeks after the first administration of famotidine; *First generation antihistamines; **Temporary use of steroids; †The patient had received pranlukast after RS virus infection.
or signs of underlying disease, including fever, signi- ficant malaise, and arthralgia.
In the acute management of urticaria, H1-receptor antagonists used included the first-generation H1-antihistamines such as cyproheptadine, clemastine, and oxatomide, and the second-generation agents ketotifen, epinastine, loratadine, and olopatadine. In the chronic phase of urticaria, first-generation as well as second-generation H1-receptor antagonists were used again (
The period from diagnosis of csU to the date of first administration of famotidine was 3.2 ± 4.0 months (range 2 days to 11 months). UAS was significantly decreased from 4.3 ± 0.8 just before administration of famotidine to 1.3 ± 1.0 on the first outpatient visit within 2 - 4 weeks after the first administration of famotidine (p < 0.0001,
No adverse effects due to concurrent administration of famotidine were observed. Furthermore, adverse effects such as drowsiness arising from H1-antihistamines were not enhanced by concurrent administration of famotidine.
Add-on use of famotidine with H1-antihistamines produ-
ced a favorable outcome in all the present pediatric patients with H1-antihistamine-refractory csU. Pediatric csU often spontaneously resolve, which would make it difficult to properly evaluate the effect of famotidine on csU. In this study, to assess urticaria symptoms correctly, UAS on the first outpatient visit was used. According to the patients’ mothers, however, every patient in this study achieved symptomatic relief such as improvement of itch and reduction of both area and number of hives within a few days after the beginning of famotidine administration, which strongly suggest that famotidine produced clinical improvement of csU rather than csU spontaneously resolved.
However, doubt exists regarding the efficacy of H2- receptor antagonists in csU. Although stimulation of H1- and H2-receptors, both of which are present in skin vessels, induces formation of erythema and wheals, H2- receptor stimulation alone does not lead to a warm sensation and itching [
As regarding the H1 antihistamines used in our patients, sedating H1-receptor antagonists were administered in both acute and chronic phase mainly in the previous clinics. Sedating H1 antihistamines can be effective and well tolerated by some individuals and use of them at night may help in producing better sleep [
LTRA is recommended as one of step-up management options. In a single case of this study, the LTRA with H1-receptor antagonist had been used but showed little benefit for csU. Of interest was that add-on use of famotidine resulted in a cure of csU in the patient. This is a single case experience and whether famotidine has a greater potency than LTRA should be further explored.
The major limitation of this study was its small sample size. Further studies enrolling a larger number of patients are required to confirm our findings. However, our results further support previous findings of the potential efficacy of add-on use of famotidine and might justify extending the range of application of H2-receptor antagonists from adults to pediatric patients with csU. In intractable csU, we often have no other alternative than immunomodulators such as oral steroids and ciclosporin. However, the present results suggest that famotidine could be used as adjunctive treatment before immunomodulating treatment.