Anti—vascular approaches to solid tumour therapy: Evaluation of vinblastine and flavone acetic acid
- 27 September 1995
- journal article
- research article
- Published by Wiley in International Journal of Cancer
- Vol. 63 (1) , 119-123
- https://doi.org/10.1002/ijc.2910630121
Abstract
Several agents have now been identified which exert their anti-tumour effects in large part via the tumour vasculature; these include TNFα and flavone acetic acid (FAA). More recently, Vincristine and Vinblastine have also been shown to cause a prolonged and selective decrease in tumour perfusion. Vinblastine, unlike FAA, causes no increase in plasma TNFα levels in mice bearing the CaNT tumour, suggesting 2 distinct mechanisms of anti-vascular activity for these structurally diverse agents. Since FAA and Vinblastine also show quite different normal tissue toxicities, which are separately dose-limiting, we have examined the strategy of combining these 2 agents. When Vinblastine preceded FAA by 24 hr or less, tumour growth delay was significantly enhanced without a concomitant increase in toxicity. The level of enhancement was not significantly reduced by a 5-fold decrease in Vinblastine dose, though any reduction in the dose of FAA caused a rapid reduction in treatment effectiveness. Investigation of the functional vasculature of treated tumours suggested that increased anti-vascular effects may contribute to the enhanced growth inhibition of the combined treatment. Our results demonstrate the potential benefit of combining 2 different classes of antivas-cular agent, using Vinblastine and FAA (or 5,6-MeXAA) as prototype drugs.Keywords
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