Journal List > Ann Dermatol > v.30(4) > 1097528

Kim, Lee, and Yun: Development of Vitiligo-Like Depigmentation after Treatment of Lentigo Maligna Melanoma with 5% Imiquimod Cream

Abstract

A 69-year-old man presented with a black irregular patch on his left cheek. Skin biopsy revealed lentigo maligna melanoma in situ. He was treated via partial excision of the melanoma, followed by the application of 5% imiquimod cream every other night for 6 to 8 hours. The patient experienced severe local inflammation accompanied by burning, edema, and erythema, as well as oozing and crusting. The patient discontinued using the imiquimod cream after 15 applications because of the inflammation. Depigmentation was noted in the treated area 3 months after the initiation of treatment with imiquimod cream. Histological examination using Melan-A staining of the depigmented area revealed an absence of melanocytes, which is consistent with vitiligo. The depigmented lesions improved considerably after a 5-year follow-up, and there was no recurrence of melanoma.

INTRODUCTION

Imiquimod, as a 5% cream, has been approved by the U.S. Food and Drug Administration for the treatment of genital and perianal warts. It is also used to treat actinic keratosis and superficial basal cell carcinoma; however, its range of applications is gradually expanding. In cases of lentigo maligna melanoma with lesions in areas where surgical intervention is not feasible, treatment with 5% imiquimod cream has been reported to have a high success rate. There is also a growing number of reports on the use of 5% imiquimod cream for the removal of residual lesions after surgery1. The following presentation is a case report of a patient with a resolving facial lentigo maligna melanoma who developed vitiligo-like depigmentation following treatment with 5% imiquimod cream.

CASE REPORT

A 69-year-old male patient presented with a black irregular patch on his left cheek. The patient had undergone laser treatment for the condition at a clinic 7 years ago; however, he had recurrences without receiving any additional treatment. At our hospital, he presented with a black patch on his left cheek measuring approximately 3.5×3.5 cm with unclear boundaries and uneven coloration (Fig. 1A). The skin biopsy identified the condition as lentigo maligna melanoma in situ. The patient was advised to undergo a skin graft or flap after a complete excision of the lesion; however, he declined this treatment to avoid scarring. The patient elected to undergo partial resection of the lesions including the darkest area (Fig. 1B), followed by the application of 5% imiquimod cream three times a week. Application of the imiquimod cream to the lesion was initiated 2 weeks after the partial resection. The cream induced a severe local inflammatory reaction, which caused burning, edema, erythema, oozing, and crusting (Fig. 2A). Because of the reaction, the use of the cream was limited to 15 applications over 3 months. Depigmented lesions were observed in the treated area 3 months after the initiation of topical imiquimod therapy (Fig. 2B). Histological examination using Melan-A staining of the depigmented area revealed the absence of melanocytes, which was consistent with vitiligo (Fig. 2C). The depigmented lesions improved greatly after a 5-year follow-up and the melanoma has not recurred (Fig. 2D). We received the patient's consent about publishing all photographic materials.

DISCUSSION

The number of reports on the use of 5% imiquimod cream for the treatment of melanoma in situ, especially lentigo maligna, is growing. Ellis et al.2 reviewed 46 previous studies in which patients with melanoma in situ were treated with imiquimod cream. The reports indicated that 220 of 264 (83.3%) patients showed clinical or histological clearance of the melanomas. Similarly, a recently published study1 indicated an overall clinical clearance rate of 86.2% was obtained at a mean follow-up of 42.1 months when 5% imiquimod cream was used as the primary or adjuvant therapy for lentigo maligna. However, there is still a lack of efficacy and safety data from randomized controlled studies on the use of imiquimod cream for treating melanoma in situ, whereas studies on palliative surgical treatment are widely available. Therefore, imiquimod cream is currently used to treat melanoma in situ on an off-label basis.
Globally, depigmentation or hypopigmentation occurring after treatment with imiquimod cream has been reported in 15 previous case reports on 17 patients. In nine of the cases, the imiquimod treatment was for genital warts or extramammary Paget's disease345678. The extragenital cases of imiquimod-induced depigmentation or hypopigmentation occurred after treatment of basal cell carcinomas at various locations including the face, chest, and upper extremities91011. However, to the best of our knowledge, no case of vitiligo has been reported after the application of imiquimod cream for melanoma treatment.
It has been shown that cryotherapy or podophyllin application for extramammary Paget's disease prior to topical imiquimod treatment results in severe irritation but no pigmentary changes36. Similarly, no pigmentary changes were observed when fluorouracil injection, trichloroacetic acid solution, or cryotherapy were used to treat genital warts prior to imiquimod treatment. Thus, pigmentary changes after imiquimod treatment are not thought to be due to hypopigmentation induced by simple skin irritation346.
Schön et al.12 reported on imiquimod-induced apoptosis in melanoma cells in vitro and in vivo. Kim et al.13 also reported that an imiquimod-induced immune response mediates vitiligo-like reactions and apoptosis in human melanocytes. Imiquimod binds to Toll-like receptors (TLR) 7 and 8. TLR7 activates the T-helper 1 response and increases the production of pro-inflammatory cytokines such as interferon alpha, tumor necrosis factor alpha, and interleukin (IL)-12, which play an important role in the pathogenesis of vitiligo14. In addition, imiquimod directly increases the expressions of pro-inflammatory cytokines such as IL-6, IL-8, and IL-10, and pro-apoptotic molecules, which can also cause vitiligo15.
In a study by Kumar and Narang7, 22 immunocompetent male patients with genital warts were treated with 5% imiquimod cream thrice weekly. However, during the 7-week follow-up period, one of the patients presented with vitiligo lesions and severe adverse reactions in the treated area. A prolonged period between the application of imiquimod cream and a follow-up visit may result in difficulty in evaluating the onset of depigmentation.
A review of related literature shows that some studies have reported a 4-week4, 8-week5, 10-week9, and 12-week610 period between the application of imiquimod cream and the onset of depigmentation. In the present case, depigmented lesions were observed prominently 3 months after the start of treatment. The vast majority of cases where there were long periods between the application of imiquimod cream and hospital revisits have reported the confirmation of depigmented lesions within 6 months of treatment3. Therefore, if a patient has esthetic outcome concerns or undergoes treatment on body areas that are easily visible, follow-up visits at short intervals within the first 3 months of treatment would be useful.
The occurrence of depigmented lesions after the application of imiquimod cream in a patient who had a family history of vitiligo has been reported4. In addition, halo nevi was reported to have occurred in areas outside the sites of imiquimod cream application8. In previous studies describing depigmented lesions due to treatment with imiquimod cream, the maximum follow-up period was 18 months. In most of those cases, there was no repigmentation; however, Stefanaki et al.4 observed a 2% repigmentation after a 3-month follow-up. In the present case, after treatment with imiquimod cream commenced, there was a follow-up treatment period of 5 years, which was much longer than that in any of the previous reports. At 5 years, more than 50% repigmentation had been achieved. In this case, we did not perform any treatments for the depigmentation, therefore, it is thought that spontaneous repigmentation of the lesions was obtained due to discontinuation from the imiquimod-induced immune response and long term follow-up.
In conclusion, vitiligo-like depigmentation occurrence after the application of imiquimod cream is one of the immunological adverse reactions that may be associated with the mechanism of action of imiquimod. But also, unlike any other vitiligo, it can show spontaneous repigmentation over time. Thus, it is important for clinicians to be aware that imiquimod cream can treat residual lentigo melanoma in situ effectively after partial excision. In addition, the development of vitiligo-like depigmentation, and then repigmentation following treatment with imiquimod cream occurs.

Figures and Tables

Fig. 1

Clinical photographs prior to and after partial excision of melanoma in situ. (A) A large black patch with an unclear boundary and uneven color on the left cheek prior to treatment. (B) Remaining black patch after partial excision of melanoma.

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Fig. 2

(A) Severe local inflammatory reaction occurred after application of 5% imiquimod cream. (B) Depigmented lesions are observed in the treated area after 3 months. (C) Histological examination using Melan-A staining of the depigmented area revealed the absence of melanocytes (×100). (D) Partial improvement in vitiligo-like depigmentation after 5-year treatment without recurrence of melanoma.

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Notes

CONFLICTS OF INTEREST The authors have nothing to disclose.

References

1. Swetter SM, Chen FW, Kim DD, Egbert BM. Imiquimod 5% cream as primary or adjuvant therapy for melanoma in situ, lentigo maligna type. J Am Acad Dermatol. 2015; 72:1047–1053.
crossref
2. Ellis LZ, Cohen JL, High W, Stewart L. Melanoma in situ treated successfully using imiquimod after nonclearance with surgery: review of the literature. Dermatol Surg. 2012; 38:937–946.
crossref
3. Brown T, Zirvi M, Cotsarelis G, Gelfand JM. Vitiligo-like hypopigmentation associated with imiquimod treatment of genital warts. J Am Acad Dermatol. 2005; 52:715–716.
crossref
4. Stefanaki C, Nicolaidou E, Hadjivassiliou M, Antoniou C, Katsambas A. Imiquimod-induced vitiligo in a patient with genital warts. J Eur Acad Dermatol Venereol. 2006; 20:755–756.
crossref
5. Senel E, Seckin D. Imiquimod-induced vitiligo-like depigmentation. Indian J Dermatol Venereol Leprol. 2007; 73:423.
crossref
6. Kwon HH, Cho KH. Induction of vitiligo-like hypopigmentation after imiquimod treatment of extramammary Paget's disease. Ann Dermatol. 2012; 24:482–484.
crossref
7. Kumar B, Narang T. Local and systemic adverse effects to topical imiquimod due to systemic immune stimulation. Sex Transm Infect. 2011; 87:432.
crossref
8. Serrão VV, Páris FR, Feio AB. Genital vitiligo-like depigmentation following use of imiquimod 5% cream. Eur J Dermatol. 2008; 18:342–343.
9. Mendonça CO, Yates VM. Permanent facial hypopigmentation following treatment with imiquimod cream. Clin Exp Dermatol. 2006; 31:721–722.
crossref
10. Jacob SE, Blyumin M. Vitiligo-like hypopigmentation with poliosis following treatment of superficial basal cell carcinoma with imiquimod. Dermatol Surg. 2008; 34:844–845.
crossref
11. Sriprakash K, Godbolt A. Vitiligo-like depigmentation induced by imiquimod treatment of superficial basal cell carcinoma. Australas J Dermatol. 2009; 50:211–213.
crossref
12. Schön MP, Wienrich BG, Drewniok C, Bong AB, Eberle J, Geilen CC, et al. Death receptor-independent apoptosis in malignant melanoma induced by the small-molecule immune response modifier imiquimod. J Invest Dermatol. 2004; 122:1266–1276.
crossref
13. Kim CH, Ahn JH, Kang SU, Hwang HS, Lee MH, Pyun JH, et al. Imiquimod induces apoptosis of human melanocytes. Arch Dermatol Res. 2010; 302:301–306.
crossref
14. Mashiah J, Brenner S. Possible mechanisms in the induction of vitiligo-like hypopigmentation by topical imiquimod. Clin Exp Dermatol. 2008; 33:74–76.
crossref
15. Dahl MV. Imiquimod: a cytokine inducer. J Am Acad Dermatol. 2002; 47:4 Suppl. S205–S208.
crossref
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Sook Jung Yun
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