Ann Dermatol. 2009 Feb;21(1):81-83. English.
Published online Feb 28, 2009.
Copyright © 2009 Korean Dermatological Association and The Korean Society for Investigative Dermatology
Case Report

Squamous Cell Carcinoma Masquerading as Rhinophyma

Min Joo Kim, M.D., Hye Sung Kim, M.D., Young Min Park, M.D. and Hyung Ok Kim, M.D.
    • Department of Dermatology, Kangnam St. Mary's Hospital, College of Medicine, The Catholic University of Korea, Seoul, Korea.
Received July 29, 2008; Accepted August 31, 2008.

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

Abstract

A rhinophyma lesion can mask the existence of coexisting occult skin cancers, and many types of tumors can mimic a rhinophyma. Although several coexistent malignant tumors have been reported in patients with rhinophyma, few reports have described the coexistence of rhinophyma and cutaneous squamous cell carcinoma (SCC). Herein, we report on a case of SCC in a 45-year-old man who presented with 2-month-history of a painful, erythematous, globular plaque on the tip of his nose and this lesion mimicked a rhinophyma lesion. The histopathologic examination showed a proliferation of atypical squamous cells that extended into the dermis, which was consistent with SCC. He was treated with surgical excision, and there has been no evidence of recurrence during the follow-up period of 1 year.

Keywords
Rhinophyma; Squamous cell carcinoma

INTRODUCTION

Rhinophyma is a kind of phymatous rosacea that occurs most often in men with thick sebaceous skin1. It is characterized by patulous follicular orifices, thickened skin and large nodulocystic lesions clustered over the distal half of the nose2. Hugely dilated follicles can also be present that contain long vermicular plugs of sebum and keratin. The histologic features are pilosebaceous gland hyperplasia with fibrosis, inflammation and telangiectasia1. The clinical diagnosis of rhinophyma is often straightforward, yet there are some cutaneous conditions that may mimic rhinophyma, including several malignant tumors. The possible clinical differentiating features between rhinophyma and malignant tumors are the drainage, ulceration and rapid growth pattern that are seen only in malignant tumors3.

In this report, we present a case of infiltrating squamous cell carcinoma (SCC) that occurred on the tip of the nose, and this lesion masqueraded as a rhinophyma.

CASE REPORT

A 45-year-old man presented with a 2-month history of an enlarging erythematous plaque on the tip of his nose. He complained of intermittent pain, but he denied pruritus or any other symptoms. He had been treated with a topical retinoid and oral doxycycline for 1 month, with no improvement. His past medical history was unremarkable, and his family history was noncontributory. The physical examination revealed a 3 cm-sized, ill-defined, erythematous, nodular plaque on the nose tip that contained telangiectasias and crusting (Fig. 1).

Fig. 1
A solitary, 3×2 cm sized, irregular shaped, erythematous, nodular plaque with telangiectasia and crusting on the tip of the nose.

A skin biopsy specimen was taken from the center of the lesion and this was stained with hematoxylin and eosin. Histologic examination demonstrated an irregular tumor mass throughout the epidermis and dermis (Fig. 2A). The epidermis was characterized by squamous dysplasia, and the invading tumor mass consisted of well-differentiated squamous cells that showed individual keratinization (Fig. 2B). Also present were tumor nests of poorly differentiated atypical squamous cells.

Fig. 2
(A) The histopathologic findings show a tumor invading into the dermis (H&E, ×40). (B) The invading tumor is composed of well-differentiated squamous cells that show individual keratinization (H&E, ×400).

The diagnosis of SCC was made based on these histopathological findings, and further imaging studies, including lung CT and PET-CT, were performed to evaluate for systemic involvement. These imaging studies showed no evidence of distant metastasis or a hidden primary malignancy. The patient was referred to a plastic surgeon, who surgically excised the lesion. No recurrence has been noted during the follow-up period of 1 year.

DISCUSSION

Wende and Bentz4 first reported a connection between malignancy and rhinophyma in 1904. Various malignancies, including basal cell carcinoma5, angiosarcoma6, SCC7-9 and sebaceous carcinoma10, have been reported to coexist with rhinophyma or to resemble it. Furthermore, it has been suggested that the incidence of certain malignancies is markedly increased in patients with rhinophyma when compared to those patients without rhinophyma11. However, there is currently insufficient evidence to suggest a secondary transformation of long-standing rhinophyma into any malignancy; it is not known whether rhinophyma predisposes a patient to any malignancy whatsoever.

The diagnosis of rhinophyma is principally based on the clinical features and it is often straightforward. However, several clinical characteristics including drainage, ulceration and a rapid growth pattern may be indicative of a malignancy3. In the previous case reports of SCC clinically associated with rhinophyma, all the patients commonly had a long-standing stationary rhinophyma (3 to 20 years) and then it showed unexpected rapid growth and ulcerative change during the several weeks preceding the diagnosis of SCC7-9. In contrast, our case is unique in that he has no previous history of rhinophyma or rosacea, and a rhinophyma-like plaque rapidly developed on the nose tip over such a short period of 2 months. The histopathologic examination revealed well-differentiated squamous cell carcinoma with no evidence of rhinophyma. Thus, as is shown by our case, the unusual growth pattern of a newly formed rhinophyma-like lesion as well as the abrupt clinical changes of a preexisting steady rhinophyma could support the possibility of hidden malignancy rather than a rhinophyma itself.

Once the pathologic diagnosis of SCC is made, a thorough examination should be performed to evaluate whether it is a primary malignancy or a metastatic lesion. In our case, subsequent imaging studies, including lung CT and PET-CT, showed no evidence of hidden primary internal malignancy, and the patient was finally diagnosed with cutaneous SCC that occurred primarily on the tip of his nose.

Primary cutaneous SCC of the nose is not uncommon, and its reported incidence has ranged from 5.8% to 7.5% of all cutaneous SCCs in Korea12-14. It is well known that chronic exposure to ultraviolet radiation is the main etiologic factor for the genesis of SCC15. Besides some acquired and genetic precancerous skin conditions, some chemical carcinogens have been reported to be involved in the development of SCCs of the nose; the incidence of SCC of the nose is remarkably higher among industrial workers coming in contact with nickel subsulphide, calcium chromate, isopropyl oil and so on16. However, this is not such a case because there was no known provoking factor for our patient.

Treatment of a squamous cell carcinoma resembling a rhinophyma is directed by the histologic diagnosis7. Non-excisional ablative techniques, Mohs surgery, conventional surgical excision and radiation therapy are generally considered for treatment17.

With respect to the anatomic site, SCCs of the nose tip are not a high risk lesion compared with SCCs of the ear or the lip17. Accordingly, rhinophyma-like clinical features do not seem to have a prognostic implication for SCCs. However, the prognosis may be poor as an unfortunate consequence of delayed treatment that's caused by the misdiagnosis of a rhinophyma when considering that rhinophyma is mostly diagnosed clinically without performing a skin biopsy.

Taken together, our case suggests that for managing the patients with a rhinophyma lesion, physicians must be aware of the possibility that the lesion is a true malignancy. Lesions on the nose should be carefully reevaluated when they show no response to conventional therapies, or when any clinical change occurs in them.

References

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