Topical Mitomycin Chemotherapy for Conjunctival Malignant Melanoma and Primary Acquired Melanosis With Atypia: Clinical Experience With Histopathologic Observations

doi:10.1001/archopht.118.7.885

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Vol. 118 No. 7, July 2000

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Topical Mitomycin Chemotherapy for Conjunctival Malignant Melanoma and Primary Acquired Melanosis With Atypia

Clinical Experience With Histopathologic Observations

Hakan Demirci, MD; Steven A. McCormick, MD; Paul T. Finger, MD

Arch Ophthalmol. 2000;118:885-891.

Objectives To clinically evaluate topical mitomycin chemotherapyin patients with diffuse, multifocal, or recurrent primary acquiredmelanosis with atypia and/or conjunctival malignant melanomaand to histopathologically study ocular tissue samples obtainedbefore and after treatment.

Methods Chemotherapy with topical mitomycin, 0.04% 4 timesdaily, was administered for 28 days as the primary and onlytreatment in 7 patients (after biopsy) and for 7 days as adjuvanttherapy to excision and cryotherapy in 5 patients. Mean follow-upwas 38 months. Five patients developed subconjunctival recurrences,for which 2 underwent orbital exenteration and 3 were treatedconservatively. Histopathologic specimens of conjunctival, adnexal,and ocular tissues obtained before and after chemotherapy wereevaluated.

Results Regression of tumor was observed in 11 patientswith primary or adjuvant topical mitomycin chemotherapy. Onepatient with nodular melanoma was resistant to mitomycin chemotherapy.Histopathologic findings included regionally variable conjunctivalepithelial atrophy and thinning. Dyskeratosis and focal keratinizationin conjunctival epithelium were noted. Epithelial nuclei wereoccasionally pyknotic in areas of atrophic epithelium. Subepithelialinflammation was present and was most intense in areas withsevere atrophy and/or keratosis. Two patients with primary treatmentand 2 with adjuvant treatment developed subconjunctival recurrence.In patients with recurrent malignant melanoma, the deeper layersof the lamina propria were involved, with sparing of the epitheliumand superficial lamina propria. Transient keratoconjunctivitiswas observed in all patients during treatment. In evaluationof the exenteration specimens, corneal, scleral, episcleral,retinal, and anterior structures were within normal limits.

Conclusions Topical mitomycin chemotherapy was found toinduce regression of conjunctival melanoma and primary acquiredmelanosis with atypia. When mitomycin chemotherapy was usedas an adjuvant to excision and cryotherapy, 2 (40%) of 5 patientsexperienced tumor recurrence at a mean of 4.3 years' follow-up.Our histopathologic findings demonstrated a long-term mitomycinchemotherapy–related effect on the conjunctiva. The degreeof chronic atrophy and inflammation was not clinically significant.The pattern of effect and location of recurrent disease suggestthat this regimen of topical mitomycin chemotherapy was mosteffective for superficial tumors. No complications that wouldpreclude use of our dose regimen were noted. Although subconjunctivalor orbital recurrences were noted, topical mitomycin chemotherapywarrants further investigation as an alternative treatment forprimary acquired melanosis with atypia and conjunctival malignantmelanoma.

From The New York Eye Cancer Center (Dr Finger) and the Departments of Ophthalmology and Pathology and Laboratory Medicine, The New York Eye and Ear Infirmary (Drs Demirci, McCormick, and Finger), New York.

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