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Wick, M.M.

L-Dopa methyl ester: prolongation of survival of neuroblastoma-bearing mice after treatment.

L-Dopa has has been shown to demonstrate enhanced toxicity toward melanoma cells in vitro. Since melanocytes arise from the neural crest embryologically, the effect of L-dopa methyl ester, a soluble analog, on the murine C1300 neuroblastoma was studied. There was significant antitumor activity against the neuroblastoma, which was enhanced by combination with a dopa decarboxylase inhibitor, Ro4-4602. In vitro studies suggested inhibition of DNA synthesis as the principal site of action. A mechanism involving sulfhydryl compound scavenging is postulated.[1]

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L-Dopa methyl ester: prolongation of survival of neuroblastoma-bearing mice after treatment. Wick, M.M. Science (1978) [Pubmed]

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