Led by Emanual Maverakis of the University of California Davis Department of Dermatology, the research found that Interleukin (IL)-2 combined with imiquimod and topical retinoid therapy in patients with so-called "in-transit metastases" is a promising therapeutic option.
"It's unclear if the recently developed targeted melanoma therapies that have revolutionised management of patients with internal melanoma metastases are useful in patients with metastatic disease limited of the skin," said Maverakis.
"Our results demonstrate that intralesional therapy with a protein that causes immune cells to divide, given in combination with a topically applied immune activator, can be a highly effective treatment for these patients," Maverakis said.
About 10 per cent of patients with advanced melanoma develop what are called cutaneous metastases, often located "in-transit" to the patients' lymph nodes.
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Historically, treatment for these metastatic lesions has been surgical excision with or without radiation therapy, but disease recurrences can still be very high.
For the study, the researchers did a retrospective analysis of patients with either stage III or stage IV melanoma who had history of treatment with IL-2 therapy combined with imiquimod and a topical retinoid.
The data indicated that all patients achieved complete clinical response to the treated lesions within one to three months of starting the intralesional IL-2-based therapy.
After two years, 82 per cent of the patients in the study were alive, and seven were alive at the conclusion of the study without melanoma recurrence. The remaining five patients died from unrelated causes.
The study was published in the Journal of the American Academy of Dermatology.