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Advances in Dermatology and Allergology/Postępy Dermatologii i Alergologii
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5/2014
vol. 31
 
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Letter to the Editor
Long-term treatment of refractory severe chronic urticaria by omalizumab: analysis of two cases

Irene Fiorino
,
Filomena Loconte
,
Anna Simona Rucco
,
Andrea Nico
,
Maddalena Vacca
,
Elisabetta Damiani
,
Eustachio Nettis
,
Maria Filomena Caiaffa
,
Luigi Macchia

Postep Derm Alergol 2014; XXXI, 5: 332–334
Online publish date: 2014/10/22
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Omalizumab is a recombinant humanized monoclonal antibody raised against the Cε3 domain of human IgE, whose efficacy and safety in the treatment of moderate to severe asthma has been demonstrated [1–3]. Several other possible indications for this innovative drug have been considered, including severe idiopathic urticaria [4–6].
Here we report on two stubbornly refractory cases successfully treated with omalizumab.
Case 1. A Caucasian housewife and part-time domestic caretaker, aged 50. Since 2002, she had been suffering from severe idiopathic urticaria. Giant, intensively itchy lesions were often (but not always) elicited by pressure.
Previous unsuccessful therapies comprised: high-dose antihistamine (including ketotifen); leukotriene modifiers; dapsone; cyclosporine (4 mg/kg/day); bromazepam; and prolonged low to mid-dose corticosteroid courses.
At presentation, the patient had been treated with betamethasone (1 mg/day) for 2 years, consecutively, in association with various antihistamines at high dosage (up to 4 times the standard dosage). Moreover, she was following a rather restricted “hypo-allergic” diet. In spite of this therapeutic regimen, she was fully symptomatic, with daily eruptions of large itchy wheals, appreciable scratching lesions, and severe pruritus. The current 7-day Urticaria Activity Score (UAS) [7] was > 38. Total IgE count was 170 kU/l. Other allergy and immunology tests were negative, including auto-immunity tests. However, the autologous serum test was positive (undiluted), compatible with the presence of possible autoimmune pathogenic mechanisms (e.g. autoantibodies to IgE or to the α chain of the high affinity IgE receptor FcεRI).
After discontinuation of the corticosteroid therapy and an additional attempt at controlling the symptoms with fexofenadine and cyproheptadine (which failed), we started the treatment with omalizumab (off-label; 300 mg/month; the dose was calculated according to the standard schedule for severe asthma; body weight was 52 kg).
The monoclonal antibody produced a dramatic and almost immediate (2 days) clinical improvement. Antihistamine therapy (fexofenadine 180 mg daily and ketotifen 2 mg b.i.d.) was initially needed in order to achieve full symptom control (7-day UAS Ξ 0). After 9 months we decided to raise the omalizumab dosage to 450 mg/month. That enabled discontinuation of the antihistamine therapy. As at March 2014, the patient has been under omalizumab treatment for 21 months and remains disease-free. No immediate or delayed side effects have been detected (54 single administrations given).
Case 2. Also a Caucasian housewife, 54, who had been suffering from severe idiopathic urticaria since she was 30, first episodically, then, since 2003, chronically. The 7-day UAS at presentation was 40. The autologous serum test was positive (undiluted). Over the time, aside from high-dose non-sedating antihistamines (up to 4 times the standard dosage), therapeutic approaches had included: prolonged corticosteroid courses; sedating H1-antihistamines; H2-antihistamines; bromazepam; cyclosporine (4 mg/kg/daily; producing unsustainable side effects); methotrexate; and high-dosage mycophenolate mofetil. All these therapies had failed. Therefore, in June 2010, we started an off-label omalizumab course at the dosage of 150 mg/month (at that time, we opted for a dosage independent from total IgE measurement (195 kU/l) and body weight (75 kg)). Also in this case, a rapid symptom relief followed and the concomitant antihistamine therapy could be first tapered and then discontinued (7-day UAS Ξ 0). The patient has been essentially disease-free for 4 years, under omalizumab treatment, with a UAS value of 0. However, we have recently decided to shorten the administration interval to 3 weeks, due to the occasional recurrence of wheals and pruritus towards the end of the previous inter-administration interval of 4 weeks.
No immediate or delayed side effects were ever noticed (49 injections administered).
Omalizumab has been regarded for some years already as a possible valuable therapeutic option for refractory severe urticaria [4–6]. Several authoritative double-blind placebo-controlled studies have been published in the last few years [8–10]. Thus, an early, phase II, dose-finding investigation showed efficacy after a single omalizumab dose of 300 mg [8]. A more recent, phase III study investigated safety of omalizumab treatment (300 mg, every 4 weeks, for 24 weeks) in patients with chronic idiopathic urticaria resistant to H1-antihistamines at up to 4 times the approved dose plus H2-antihistamines and leukotriene antagonists. Along with an excellent safety profile, this study also showed that omalizumab was robustly efficacious [9]. Another phase III study was carried out in patients who remained symptomatic in spite of H1-antihistamines at licensed doses. The patients received 3 injections of omalizumab, spaced 4 weeks apart, at doses of 75 mg, 150 mg, and 300 mg or placebo. The study showed a significant improvement in patients receiving 150 mg or 300 mg of omalizumab (but not 75 mg), as compared with placebo [10].
Moreover, several cases of off-label treatment, including case reports and small and middle-sized series [11–14] have been published.
Taken together, this literature indicates that this novel approach is more than realistic and feasible.
However, many aspects of the problem remain to be assessed, as epitomized by the fact that, so far, omalizumab has not been approved for urticaria (of any kinds), worldwide. In particular, retrospective studies, conducted in real-life settings [15, 16], have started to address such important issues as treatment duration, long-term efficacy and safety, dose adjustment, and others.
In this context, we believe that these two additional cases, managed for prolonged periods of time, are likely to provide further noteworthy information, which can be synthesized as follows: Omalizumab was effective, enabling achievement of complete control in these stubbornly recalcitrant cases, characterized by severe symptoms lasting for many years and resistant to virtually all known treatments. The relief afforded was impressively fast, as reported also by others [15]. This may suggest that omalizumab efficacy might be investigated also in the case of aggressive, treatment-resistant acute urticaria, perhaps with a single administration followed by conventional therapy. It seemed that the dosage had to be determined empirically (rather than rigidly based on total IgE levels and body weight, as for severe asthma) and, perhaps, adjusted, from time to time, in order to achieve and maintain full disease control, as recently suggested [16]. Prolonged treatment did not seem to cause a decline in efficacy. On the other hand, it appeared that omalizumab should be given for very long periods of time, if not indefinitely, in cases such as those presented [9]. The safety profile was excellent, since neither immediate nor delayed side effects of any kinds were recorded, over many months. Finally, lack of omalizumab approval for this specific indication by regulatory boards precludes a wider and probably highly beneficial employment of omalizumab in patients with severe chronic urticaria, which, in our opinion, would lead to a net reduction in both the human and the social and economic burden of this disease.
The study was approved by the Ethics Committee of one of the two Institutions involved (University of Foggia) and complies with the provisions of the Declaration of Helsinki (and subsequent amendments). Informed consent was granted by the two participants.

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