Abstract
Introduction
5-Fluorouracil is a fluoropyrimidine antineoplastic medication that is used to topically treat actinic keratoses. Although local adverse effects to the drug are common and anticipated, distant skin reactions are rare and unexpected. In this case report, we describe a patient who developed seborrheic dermatitis-like eruption at a distant site after topical application of 5-fluorouracil to his arms.
Case report
A 63-year-old man with actinic keratoses on his arms developed a facial seborrheic dermatitis-like reaction after topically applying 5-fluorouracil 5% cream twice daily to actinic keratoses on his forearms for 7 days. The facial dermatosis resolved shortly after discontinuation of the 5-fluorouracil; upon rechallenge of topical 5-fluorouracil on his arms, the facial seborrheic dermatitis recurred.
Discussion
Several case reports have been published which describe exacerbations of preexisting seborrheic dermatitis with local topical 5-fluorouracil. Additionally, one case series describes the development of scrotal dermatitis in two patients after distant treatment with 5-fluorouracil. The pathogenesis that causes this distant reaction is unclear.
Conclusion
We describe a patient with a seborrheic dermatitis eruption after topical application of 5-fluorouracil at a distant site. The etiologic association between the drug and adverse effect was confirmed with multiple cycles of application and discontinuation of the offending agent.
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Introduction
5-Flurouracil is a pyrimidine antimetabolite; topical preparations of this agent are used in the treatment of actinic keratosis [1]. Seborrheic dermatitis is an inflammatory papulosquamous dermatosis, and although it may affect the scalp and anterior chest, many patients exhibit only facial manifestations of this condition [2]. Herein we describe a man with actinic keratoses on his arms, and no similar lesions or history of seborrheic dermatitis on his face, who developed a facial seborrheic dermatitis-like dermatosis after applying 5-fluorouracil topically to actinic keratoses on his arms. We also review seborrheic dermatitis-like eruptions secondary to systemic or topical 5-fluorouracil.
Informed consent was obtained from the participant for being included in the study.
Case Report
A 63-year-old man presented for evaluation and treatment of asymptomatic lesions on his distal upper extremities. His past medical history was significant for nephrolithiasis and hypertension, for which he had been taking amlodipine and triamterene–hydrochlorothiazide for many years. He also had a history of a basal cell carcinoma and a squamous cell carcinoma on his arms; both were excised 5 years earlier, and there has been no recurrence. The patient had scaling of his eyebrows 20 years ago which had spontaneously resolved; he otherwise had no prior history of seborrheic dermatitis. He had no recent sunburn or rash on his face.
Cutaneous examination showed erythematous scaly plaques on his bilateral forearms from just above the elbow to the dorsal hands. There was no scaling or erythematous lesions on his scalp, face, chest, or back. Based on clinical morphology, the diagnosis of actinic keratoses was established.
After a discussion of treatment options, including liquid nitrogen cryotherapy, photodynamic therapy, and topical agents (diclofenac, 5-fluorouracil, imiquimod, or ingenol mebutate), the patient elected to proceed with topical 5-fluorouracil 5% treatment. The initial treatment was twice daily for 7 days to be repeated every 2 months until his 6-month follow-up visit. He had an excellent response to treatment, with erythema and crusting of his actinic keratoses after the first treatment. At completion of therapy, mupirocin 2% ointment was used twice daily until the area returned to normal.
Four and six months after the follow-up appointment, the patient retreated the forearm actinic keratoses with 5-fluorouracil 5% cream twice daily. On the seventh day of therapy in each treatment cycle, he noted asymptomatic erythema and scaling on his face. Cutaneous examination revealed erythematous scaling plaques involving the glabellar areas, malar cheeks, paranasal regions, upper lip, and perioral region with extension to the chin (Fig. 1). His arms showed hyperpigmentation in sun-exposed areas on his arms bilaterally. There was diffuse scaling and superficial desquamation of the extensor forearms bilaterally (Fig. 2).
The 5-fluorouracil was discontinued, and mupirocin 2% ointment was applied to the forearms twice daily. Both arms and face promptly returned to their normal appearance, the latter without topical intervention.
Laboratory evaluation revealed normal complete blood cell count, including white blood cell count. His serum chemistries, including liver function, were normal. Evaluation of dihydropyrimidine dehydrogenase (DPD) enzyme showed a normal genotype. The three most common variants that have been consistently associated with 5-fluorouracil toxicity are c.1679T > G, c.2846A > T, and c.1905 + 1G > A [3, 4]; none of these gene mutations were detected in this individual.
Correlation of the history and morphologic features established a diagnosis of seborrheic dermatitis-like eruption on the face secondary to topical application of 5-fluorouracil at the distant site of his bilateral forearms. The patient had elected to challenge the initial observation with repeated treatment, which resulted in similar consequences, confirming the suspicion that the reaction was caused by 5-fluorouracil.
Despite the repeated development of seborrheic dermatitis-like facial eruption after applying 5-fluorouracil, the patient was curious about this adverse effect. Therefore, 2 months later, he elected to treat his buttocks twice daily with 5-fluorouracil. After 5 days of therapy, there was no reaction on his buttocks or his face, so he discontinued the medication.
He subsequently proceeded to again treat his forearm actinic keratoses. However, since the facial eruption had occurred after 7 days of therapy, he only treated his forearms for 5 days. During the fourth day of application, he developed similar erythematous plaques and scaling on his face with this shortened treatment regimen. The 5-fluorouracil was stopped on the fifth day, and the seborrheic dermatitis slowly resolved.
Discussion
5-Fluorouracil is an antineoplastic agent. As a uracil analog, the drug inhibits both DNA and RNA synthesis by preventing the incorporation of uracil into RNA, and it also inhibits thymidylate synthase, an enzyme required for converting deoxyuridine monophosphate to deoxythymidine monophosphate, a component of DNA [1].
Systemic 5-fluorouracil has been used as an integral component of monotherapy or combination chemotherapy in patients with either colon or breast cancer [5]. It was observed that patients treated with systemic 5-fluorouracil developed inflammation and then resolution of actinic keratoses; this prompted the development of topical 5-fluorouracil for this skin condition [6, 7].
Metabolism of 5-fluorouracil is dependent upon its degradation by dihydropyrimidine dehydrogenase, an enzyme encoded by the DPYD gene that reduces 5-fluorouracil to the inactive dihydrofluorouracil [8]. In patients with a deficiency or abnormal variants of DPYD, the response to 5-fluorouracil is greater. Similarly, the adverse effects are also more prominent [3].
Topical 5-fluorouracil is associated with the following cutaneous adverse effects: allergic contact dermatitis, conjunctivitis, corneal irritation, erosions, hyperpigmentation, hypopigmentation, irritant dermatitis, onycholysis, photosensitivity, and secondary bacterial infections [9,10,11]. There are also several reports of individuals with a prior history of facial seborrheic dermatitis or rosacea experiencing a flare of their dermatosis after application of 5-fluorouracil to their face [12,13,14]. Systemic 5-fluorouracil has also been associated with flares of seborrheic dermatitis, particularly in patients who have active dermatitis or a history of the condition [15, 16]. Seborrheic dermatitis eruptions have also been observed in patients treated with other systemic antineoplastic agents (Table 1) [13, 16,17,18,19,20,21,22,23,24,25,26].
Our patient is unique in that he had no prior history of seborrheic dermatitis and had no previous actinic keratoses on his face. However, he developed a seborrheic dermatitis-like dermatosis on his face after application of topical 5-fluorouracil at the distant site of his forearms; there was no inadvertent application of the medication to his face. He was very pleased with the efficacious response of the 5-fluorouracil treatment to his forearm actinic keratoses and therefore elected to repeat the treatment; recurrence of the seborrheic dermatitis-like dermatosis after rechallenge with topical 5-fluorouracil confirmed the suspected etiologic association. Based upon the Naranjo adverse drug reaction probability scale, our patient’s score is 7, which indicates a probable association between the drug and adverse event [27].
The development of a dermatosis at a distant site without concurrent actinic keratoses after application of topical 5-fluorouracil is unusual. However, Shelley and Shelley described a similar phenomenon in men who were applying topical 5-fluorouracil to their face, arms, or legs and subsequently developed dermatitis of their scrotums [28]. At least two of the four men had not inadvertently applied the medication to their scrotum or to skin that came in contact with the scrotum. Similar to our patient, the cutaneous adverse event occurred on the skin that had not previously experienced dermatosis and did not have actinic keratoses; in addition, there was no history of sun exposure to the affected area of the scrotum [28].
Low or deficient DPD activity is estimated to have a prevalence of 3–5% in the general population [29]. Reduced DPD activity results in increased serum concentrations of 5-fluorouracil, thus increasing the risk of severe and sometimes lethal adverse effects, including central neurotoxicity, diarrhea, mucositis, neutropenia, and thrombocytopenia [30]. However, the DPD genotype in our patient was normal. A DPD evaluation was not performed in the patients described by Shelley and Shelley [28].
Conclusions
Topical 5-fluorouracil has been associated with adverse cutaneous side effects. Albeit infrequently reported, application of the agent to the face in patients with active actinic keratoses or a history of actinic keratoses may exacerbate the underlying condition. However, our patient’s presentation is unique since he developed the seborrheic dermatitis-like dermatosis following treatment of his forearms—a distal site without any inadvertent contact with his face—and despite an absence of prior facial dermatitis.
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Tyler Werbel and Philip R. Cohen have nothing to disclose with regards to the publication of this article.
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Werbel, T., Cohen, P.R. Topical Application of 5-Fluorouracil Associated with Distant Seborrheic Dermatitis-like Eruption: Case Report and Review of Seborrheic Dermatitis Cutaneous Reactions after Systemic or Topical Treatment with 5-Fluorouracil. Dermatol Ther (Heidelb) 8, 495–501 (2018). https://doi.org/10.1007/s13555-018-0253-2
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DOI: https://doi.org/10.1007/s13555-018-0253-2