Adjuvant pegylated interferon α-2b therapy for melanoma

Although adjuvant high-dose interferon alpha-2b therapy significantly improves 'recurrence-free survival vs observation in high-risk resected melanoma, the overall survival benefit is presently unclear Pegylation of interferon alpha-2b (peginterferon alpha-2b) allows for a reduction in the dosing frequency with increased drug exposure Adjuvant peginterferon alpha-2b therapy has also been shown to provide a significant, sustained improvement in recurrence-free survival compared with observation in patients with stage III melanoma We report on the use of adjuvant peginterferon alpha-2b; (3 mu g/kg/week) in clinical practice in a series of 8 patients treated at the Universitatsklinikum Essen in Germany following complete resection of primary melanoma at intermediate- and high-risk of recurrence (stage II-III) Treatment duration ranged from 2 to 29 months, with 4 patients receiving long-term therapy (>= 24 months) Following treatment, 5 patients (stage II) remained disease-free at 33, 33, 37, 39 and 43 months from the time of diagnosis In 2 patients, peginterferon alpha-2b was terminated 4 and 9 months after treatment initiation due to disease progression Once-weekly subcutaneous administration of peginterferon alpha-2b was convenient in all patients In 3 patients experiencing adverse events, dose reductions led to a resolution of symptoms and enabled treatment to continue long-term Three further patients discontinued therapy due to adverse events at 2, 8 and 27 months of therapy (persistent elevation of gamma-glutamyl transpeptidase, liver transaminase elevation and urosepsis) dose modifications were not applicable in these patients Thus, long-term adjuvant peginterferon alpha-2b therapy was feasible in the clinical practice setting and was generally well tolerated in these intermediate- and high-risk melanoma patients