Información de la revista
Vol. 115. Núm. 9.
Páginas 931-932 (octubre 2024)
Compartir
Compartir
Descargar PDF
Más opciones de artículo
Vol. 115. Núm. 9.
Páginas 931-932 (octubre 2024)
Case and Research Letter
Acceso a texto completo
Solar Urticaria and Omalizumab: A Retrospective Case–Control Study and Follow-Up
Urticaria solar y omalizumab. Estudio retrospectivo de casos y controles y seguimiento
Visitas
1858
A. Casanova-Esquembre
Autor para correspondencia
avonasac.94@hotmail.com

Corresponding author.
, J. Lorca-Spröhnle, R. Peñuelas-Leal, A. Pérez-Ferriols
Dermatology Department, Hospital General Universitario de Valencia, Spain
Contenido relacionado
A. Casanova-Esquembre, J. Lorca-Spröhnle, R. Peñuelas-Leal, A. Pérez-Ferriols
Este artículo ha recibido
Información del artículo
Texto completo
Bibliografía
Descargar PDF
Estadísticas
Tablas (1)
Table 1. Clinical and epidemiological characteristics of control and case patients.
Texto completo
To the Editor,

Solar urticaria (SU) is a rare chronic inducible urticaria. The management of SU is challenging, with only one small clinical trial and case series reporting variable outcomes with omalizumab.1,2

We conducted a single-center, retrospective case-control study of patients with SU on omalizumab. The primary endpoint was to find clinical, photo-biological, or serological differences that could help us predict which patients have more chances of resorting to omalizumab. The clinical response was evaluated using the Urticarial Control Test (UCT). Complete clinical response (CCR) was defined as 16 points on the UCT.3 We used the SPSS statistics software, and Fisher's exact test and the Mann–Whitney U test for qualitative and quantitative variables, respectively. All patients underwent baseline photo-testing according to the protocols drafted by the AEDV Spanish Photobiology Group.4

A total of 59 patients with SU were seen from January 2015 to December 2021. Thirteen patients (22%) needed treatment with omalizumab after failed antihistamine therapy (case group). Thirteen out of the remaining 46 patients were randomly selected (control group) by the computer program, Random Generator. The mean age was similar, 36.4 years in the case group vs 35 years in the control one. Similar results were found in both groups regarding phototype, history of atopy and clinical presentation. We obtained 3 important results: first, the most widely implicated light spectrum was visible light in both groups, but on a higher rate in the case group (76.9% vs 46.2%). Regarding phototest results, the case group had more patients with positive phototests in all wavelengths (23.1% vs 7.7%). In contrast, the control group had more patients with negative phototests (38.5% vs 7.7%). Finally, we saw differences in IgE levels: 77% of the patients in the case group showed abnormal IgE levels with mean levels of 350IU/mL vs 53.8% with mean levels of 197IU/mL in the control group. None of the differences mentioned above were statistically significant (Table 1).

Table 1.

Clinical and epidemiological characteristics of control and case patients.

  Control (n) [n=13]  Case (n) [n=13]  p 
Age (years)  36.38a±14.327b  35a±11.95b  .739d 
Phototype  I 0% (0c)II 30.8% (4c)III 46.2% (6c)IV 0% (0c)V 0% (0c)VI 0% (0c)Lost 23.1% (3cI 0% (0c)II 30.8% (4c)III 30.8% (4c)IV 7.7% (1c)V 0% (0)VI 0% (0)Lost 30.8% (4c.4944e 
UVB positive  23.1% (3c38.5% (5c.673e 
UVA positive  15.4% (2)  46.2% (6)  .202e 
VL positive  46.2% (6)  76.9% (10)  .226e 
Phototest results  UVB− UVA− VL− 38.5% (5)UVB− UVA− VL+ 38.5% (5)UVB+ UVA− VL− 7.7% (1)UVB+ UVA+ VL− 7.7% (1)UVB+ UVA+ VL+ 7.7% (1)  UVB− UVA− VL− 7.7% (1)UVB− UVA− VL+ 46.2% (6)UVB− UVA+ VL− 7.7% (1)UVB+ UVA+ VL− 15.4% (2)UVB+ UVA+ VL+ 23.1% (3)  .321e.543e.345e.476e 
IgE serum levels (median)  197.54±232.395  350.25±343.432  .142d 
IgE serum (normal/high)  Normal 46.15% (6)High 53.38% (7)  Normal 15.4% (2)High 76.9% (10)Lost 7.7% (1)  .378e 
Skin clinic  Non-photoexposed areas 38.4% (5)Photoexposed areas 61.5% (8)  Non-photoexposed areas 53.8% (7)Photoexposed areas 46.1% (6)  .431e 
Atopic associated disorders  38.5% (5)  46.2% (6)  .543e 

The statistical program SPSS, Fisher's exact test and the Mann–Whitney U test were used for qualitative and quantitative variables, respectively.

a

Arithmetic mean.

b

Standard deviation.

c

Absolute number of patients.

d

Mann–Whitney U test.

e

Fisher's exact test.

On the other hand, we studied the course of the disease of 10/13 patients who had been on a 1-year course of omalizumab. Mean follow-up was 35 months. Nine of the patients achieved CCR with 300mg every 4 weeks. Among them, 4 patients achieved CCR with de-intensification dosage (300mg every 6 weeks). De-intensification occurred 6 months (minimum) after achieving CCR and after a whole summer on therapy. Before de-intensification, the 4 patients were treated for 6, 12, and 18 months, respectively, with omalizumab 300mg every 4 weeks. None of the patients achieved CCR with omalizumab 300mg every 8 weeks. No adverse events were reported, and none of the patients discontinued treatment.

We have found more photosensitivity and higher IgE levels in patients on omalizumab than in the control group. We should mention that the IgE levels reported in the case group were slightly higher than those seen in a large serie of patients with SU in the scientific medical literature currently available.5 The rates of CCR were similar to those reported in former studies, but we obtained higher rates of CCR with de-intensified dosage (300mg of omalizumab every 6 weeks).6

Out study has some limitations such as its retrospective design and limited number of patients, which complicates finding statistically significant differences. Prospective, multicenter studies would be necessary to verify our results.

Omalizumab could be the second therapeutic step in patients with SU, with similar dosage as chronic spontaneous urticaria, with the possibility of intensification/de-intensification.

Conflict of interests

The authors declare that they have no conflict of interest.

References
[1]
I. Snast, N. Kremer, M. Lapidoth.
Omalizumab for the treatment of solar urticaria: case series and systematic review of the literature.
J Allergy Clin Immunol Pract, 6 (2018), pp. 1198-1204
[2]
P. Chicharro, P. Rodríguez, D. de Argila.
Omalizumab en el tratamiento de la urticaria crónica inducible.
Actas Dermosifiliogr, 108 (2017), pp. 423-431
[3]
T. Zuberbier, A.H. Abdul Latiff, M. Abuzakouk, S. Aquilina, R. Asero, D. Baker, et al.
The international EAACI/GA2LEN/EuroGuiDerm/APAAACI guideline for the definition, classification, diagnosis, and management of urticarial.
Allergy, (2021), pp. 1-33
[4]
A. Pérez Ferriols, J. Aguilera, P. Aguilera, D. de Argila, M.A. Barnadas, X. de Cabo, et al.
Determination of minimal erythema dose and anomalous reactions to UVA radiation by skin phototype.
Actas Dermosifiliogr, 105 (2014), pp. 780-788
[5]
A. Pérez-Ferriols, M. Barnadas, J. Gardeazábal, D. de Argila, J.M. Carrascosa, P. Aguilera, et al.
Solar urticaria: epidemiology and clinical phenotypes in a spanish series of 224 patients.
Actas Dermosifiliogr, 108 (2017), pp. 132-139
[6]
D. Morgado-Carrasco, M. Giácaman-Von der Weth, X. Fustá-Novell, S. Podlipnik, A. Pérez-Ferriols, P. Aguilera.
Clinical response and long-term follow-up of 20 patients with refractory solar urticaria under treatment with omalizumab.
Copyright © 2024. AEDV
Descargar PDF
Idiomas
Actas Dermo-Sifiliográficas
Opciones de artículo
Herramientas
es en

¿Es usted profesional sanitario apto para prescribir o dispensar medicamentos?

Are you a health professional able to prescribe or dispense drugs?