Journal Information
Vol. 96. Issue 3.
Pages 372-376 (1 May 2021)
Visits
6513
Vol. 96. Issue 3.
Pages 372-376 (1 May 2021)
Research Letter
Open Access
Randomized controlled study comparing the use of diphencyprone and anthralin in the treatment of extensive chronic alopecia areata
Visits
6513
Vanessa Barreto Rochaa,b,
Corresponding author
vanessabarreto.vbr@gmail.com

Corresponding author.
, Priscila Kakizakia,b, Aline Donatib, Carla Jorge Machadoc, Mario Cezar Piresa, Leticia Arsie Continb
a Instituto de Assistência Médica do Servidor Público Estadual, São Paulo, SP, Brazil
b Hospital do Servidor Municipal de São Paulo, São Paulo, SP, Brazil
c Departamento de Saúde Pública, Faculdade de Medicina, Universidade Federal de Minas Gerais, Minas Gerais, MG, Brazil
This item has received

Under a Creative Commons license
Article information
Full Text
Bibliography
Download PDF
Statistics
Figures (2)
Tables (1)
Table 1. Clinical, epidemiological data and comparison regarding hair regrowth in the DPCP and anthralin groups.
Full Text
Dear Editor,

Alopecia Areata (AA) does not have a well-established etiopathogenesis and its treatment, especially in the chronic form, remains a challenge.1

Its clinical spectrum varies from a single plaque to total alopecia (total AA [TAA]) or universal alopecia (UAA) when it affects all body hair. The percentage of hair loss is one of the unquestionable prognostic factors and can be measured using the SALT (Severity of Alopecia Tool) score.2,3 UAA and TAA are the types that are most refractory to treatment, and their spontaneous hair regrowth rate is less than 10%.4

Diphencyprone (DPCP) is one of the most studied treatments for extensive AA, applied weekly, usually by the doctor.5 Anthralin is an old drug, which is used at home and has a lower cost, with few studies carried out on its use in AA.6–10 Both medications act by inducing eczema over the alopecic area, with DPCP causing allergic contact dermatitis (CD) and anthralin, irritative CD.

Therefore, it can be assumed that the results of the two drugs are similar; however, there are no studies comparing the effectiveness of anthralin and DPCP in the treatment of AA.

The aim of this study was to compare the efficacy, tolerability, and safety of the two drugs in the treatment of chronic extensive AA (more than one year of duration).

A randomized, controlled clinical trial was performed at the Dermatology Trichology Outpatient Clinic at the Hospital do Servidor Público Municipal de São Paulo - Brazil. After approval by the Ethics Committee (CAAE nº 60888516.1.0000.5442) and signature of the informed consent form, 24 patients who had AA for more than one year, SALT score ≥50, and more than 30 days without treatment, were included and randomly allocated for receiving DPCP (n = 13) (with gradual dose increase until mild eczema was attained) or 2% anthralin in petroleum jelly for 30 min (n = 11). There was an intra-patient control through the initial application only in the right hemicranium. The percentage of hair regrowth was calculated through photos, by a single examiner who was blinded to the treatment group. Because of the characteristics of the medications, it was not possible for the professional applying the medication or the patient to be blinded to the substance used.

The evaluations were carried out at three months, or when there was initial hair regrowth, then at six months. The proposed treatment time was 24 weeks.

The study was funded by the Dermatology Support Fund of the Brazilian Society of Dermatology (FUNADERM).

Out of the 24 patients included, three had total AA (12.5%), 13 UAA (54.2%) and eight had extensive multifocal AA (33.3%). Clinical, demographic, and hair regrowth data are shown in Table 1.

Table 1.

Clinical, epidemiological data and comparison regarding hair regrowth in the DPCP and anthralin groups.

Variable  DPCP, n (%)  Anthralin, n (%) 
Sex  11F / 2M  10F / 1M  >0.999 
Age, mean (DP)  36.8 (10.7)  34.1 (7.0)  0.474 
Clinical type       
Multifocal  0.093 
TAA  0.642 
UAA  0.392 
Age at the 1st episode, mean (SD)  23.7 (14.8)  17.8 (11.3)  0.293 
Episode duration in months       
Median (IQR)  36 (108)  24 (102)  0.675
Minimum/Maximum  8/192  8/240 
Atopy  4 (30.8)  5 (45.5)  0.675 
Ungual alterations  3 (23.1)  3 (27.3)  >0.999 
Anti-H1 use  2 (15.4)  1 (9.1)  >0.999 
Previous treatments       
Oral corticoid  8 (61.5)  8 (72.7)  0.562 
Corticoid infiltration  6 (56.2)  8 (72.7)  0.240 
Topical corticoid  7 (43.8)  4 (36.4)  0.444 
Minoxidil  5 (38.5)  7 (63.6)  0.414 
IV Corticoid  1 (7.7)  0 (0.0)  >0.999 
Anthralin  1 (7.7)  2 (18.2)  0.576 
DPCP  2 (15.4)  3 (27.3)  0.630 
Methotrexate  1 (7.7)  3 (27.3)  0.300 
Chloroquine  0 (0.0)  1 (9.1)  0.458 
Results       
Initial SALT score       
Median (IQR)  98 (28.5)  10 (7.2)  0.178
Minimum / Maximum  60.1 / 100  93.4 / 100 
6-month SALT score       
Median (IQR)  89.9 (29.0)  99.9 (0.72)  0.242
Minimum / Maximum  60.9 / 100  75.1 / 100 

SDP, Standard Deviation; IQR, Interquartile Range; Anti-H1, Anti-Histaminic drugs; IV, Intravenous.

To compare the means, Student’s t test was used for independent samples; the non-parametric Wilcoxon and Mann-Whitney test was used to compare the medians. To compare proportions, Fisher's exact test was performed. All analyses were performed considering Intention-to-Treat (ITT) and per protocol. The level of significance was set at 5% (p < 0.05; two-tailed test).

As for hair regrowth, the improvement was small and similar in the DPCP and anthralin groups (Figs. 1 and 2). The group treated with DPCP showed some hair regrowth in 38.5% of the cases (5/13) and the anthralin group in 18.2% (2/11), a difference without statistical significance (p > 0.05). No patient had more than 75% of hair regrowth in this study. The side effects were similar in both groups (p = 0.121 for 3 months and p = 0.617 for 6 months).

Figure 1.

(A and B) DPCP – initial appointment; (C and D) DPCP – 17 applications. The patient was treated with 17 applications of DPCP and presented hair regrowth. (A and B) Initial assessment; (C and D) after 17 applications of DPCP.

(0.2MB).
Figure 2.

Anthralin: (A and B) Initial pictures; (C and D) after 24 weeks of treatment. Patient was treated with Anthralin for 24 weeks. (A and B) Initial assessment; (C and D) after 24 weeks of treatment.

(0.15MB).

A recent review found 31 studies using DPCP to treat AA, with 1,638 treated patients, but none of them were randomized or placebo-controlled studies. There was no hair regrowth in 30.7% (22.9% –39.6%) for patients with TAA and UAA, similar to that found in our group.5 In this review, the incidence of severe eczema was 30.8%, followed by lymphadenomegaly (25.8%), generalized eczema (15.8%), hyperchromia (12.7%), and influenza-like symptoms (11.1 %).5

In our case series with DPCP, only one patient had moderate eczema and two had urticaria.

Three patients were lost of follow up in the DPCP group, due mostly to problems with coming to the clinic weekly. Of the 13 patients treated with DPCP, seven finished the 24 weeks of application, with an average of 18.4 sessions.

Anthralin is used both in children and adults with AA but there have been few studies on its use, which were mainly conducted in adults.6–10 Özdemir and Balevi (2017) treated 30 children (6.7% with UAA and 3.3% with TAA) with 1% anthralin in one hemicranium for 20–60 min daily. The onset of hair regrowth was observed on average after three months of treatment, and the maximum response after nine months. Eleven patients (36.6%) attained a partial response. Nine patients (30%) who did not respond to treatment after nine months were excluded from further statistical analysis. Patients who did not respond had a higher average SALT score than those who responded completely or partially.8

As for anthralin, in our study, two patients (18.2%) showed some improvement in the SALT score. The 11 patients had erythema and pruritus, which were generally mild, and only one had moderate eczema. Most had scalp hyperpigmentation, an expected fact and a sign of adherence to treatment, which reversed a few weeks after anthralin discontinuation. In this group, two patients were lost, one due to disease activity, with significant worsening of alopecia, and the other due to personal problems.

As study limitations, this is a small sample, justified by difficulties in patient selection and the project budget. The literature has been working with small samples due to the aforementioned difficulties.5 The time of follow-up was short, only six months, often due to the participants' impatience and anxiety, who requested a change of treatment after this period.

The extent of alopecia in the groups of this study may justify the low response observed. The studied population is the one with the worst prognosis and without concomitant treatment, unlike most studies in the literature.

Although a longer time of follow-up was not achieved, this is the first prospective study comparing the effectiveness of DPCP and anthralin. In conclusion, there was no statistical difference between the responses to both treatments.

Financial support

FUNADERM - Fundo de Apoio à Dermatologia.

Authors’ contributions

Vanessa Barreto Rocha: Statistical analysis; design and planning of the study; drafting and editing of the manuscript; collection, analysis, and interpretation of data; effective participation in research orientation; intellectual participation in the propaedeutic and/or therapeutic conduct of studied cases; critical review of the literature.

Priscila Kakizaki: Approval of the final version of the manuscript; design and planning of the study; data collection; intellectual participation in the propaedeutic and/or therapeutic conduct of studied cases; critical review of the manuscript.

Aline Donati: Statistical analysis; approval of the final version of the manuscript; design and planning of the study; analysis and interpretation of data; effective participation in research orientation; intellectual participation in the propaedeutic and/or therapeutic conduct of studied cases; critical review of the literature; critical review of the manuscript.

Carla Jorge Machado: Statistical analysis; approval of the final version of the manuscript; design and planning of the study; analysis and interpretation of data; effective participation in research orientation; critical review of the manuscript.

Mario Cezar Pires: Approval of the final version of the manuscript; effective participation in research orientation; intellectual participation in the propaedeutic and/or therapeutic conduct of studied cases; critical review of the manuscript.

Leticia Arsie Contin: Approval of the final version of the manuscript; design and planning of the study; drafting and editing of the manuscript; collection, analysis, and interpretation of data; effective participation in research orientation; critical review of the manuscript.

Conflicts of interest

None declared.

Acknowledgements

To pharmacist Karina de Sá Pedras, from the Amphora Compounding Pharmacy, for supplying anthralin below the cost price, and for standardizing the supplied material, always using the same batch, packer and packaging type.

References
[1]
H.R. You, S.J. Kim.
Factors Associated with Severity of Alopecia Areata.
Ann Dermatol, 29 (2017), pp. 565-570
[2]
A. Tosti, S. Bellavista, M. Iorizzo.
Alopecia areata: a long-term follow-up study of 191 patients.
J Am Acad Dermatol, 55 (2006), pp. 438-441
[3]
E.A. Olsen, M.K. Hordinsky, V.H. Price, J.L. Roberts, J. Shapiro, D. Canfield, et al.
Alopecia areata investigational assessment guidelines – Part II. National Alopecia Areata Foundation.
J Am Acad Dermatol, 51 (2004), pp. 440-447
[4]
A. Alkhalifah, A. Alsantali, E. Wang, K.J. McElwee, J. Shapiro.
Alopecia areata update: part I. Clinical picture, histopathology, and pathogenesis.
J Am Acad Dermatol, 62 (2010), pp. 177-188
[5]
S. Lee, B.J. Kim, Y.B. Lee, W.S. Lee.
Hair Regrowth Outcomes of Contact Immunotherapy for Patients With Alopecia Areata: A Systematic Review and Meta-analysis.
JAMA Dermatol, 154 (2018), pp. 1145-1151
[6]
V.C. Fiedler-Weiss, C.M. Buys.
Evaluation of anthralin in the treatment of alopecia areata.
Arch Dermatol, 123 (1987), pp. 1491-1493
[7]
I. Duarte, J. Yoshino.
Treatment of alopecia areata with anthralin: comparative study of results obtained among children and adults.
An Bras Dermatol, 70 (1995),
[8]
M. Özdemir, A. Balevi.
Bilateral Half-Head Comparison of 1% Anthralin Ointment in Children with Alopecia Areata.
Pediatr Dermatol, 34 (2017), pp. 128-132
[9]
M.R. Ngwanya, N.A. Gray, F. Gumedze, A. Ndyenga, N.P. Khumalo.
Higher concentrations of dithranol appear to induce hair growth even in severe alopecia areata.
Dermatol Ther, 30 (2017),
[10]
V.C. Fiedler, A. Wendrow, G.J. Szpunar, C. Metzler, R.L. DeVillez.
Treatment-resistant alopecia areata. Response to combination therapy with minoxidil plus anthralin.
Arch Dermatol, 126 (1990), pp. 756-759

How to cite this article: Rocha VB, Kakizaki P, Donati A, Machado CJ, Pires MC, Contin LA. Randomized controlled study comparing the use of difenciprone and anthralin in the treatment of extensive chronic alopecia areata. An Bras Dermatol. 2021;96:372–6.

Study conducted at the Hospital do Servidor Municipal de São Paulo, São Paulo, SP, Brazil.

Copyright © 2021. Sociedade Brasileira de Dermatologia
Download PDF
Idiomas
Anais Brasileiros de Dermatologia
Article options
Tools
en pt
Cookies policy Política de cookies
To improve our services and products, we use "cookies" (own or third parties authorized) to show advertising related to client preferences through the analyses of navigation customer behavior. Continuing navigation will be considered as acceptance of this use. You can change the settings or obtain more information by clicking here. Utilizamos cookies próprios e de terceiros para melhorar nossos serviços e mostrar publicidade relacionada às suas preferências, analisando seus hábitos de navegação. Se continuar a navegar, consideramos que aceita o seu uso. Você pode alterar a configuração ou obter mais informações aqui.