Fulcover, a common triazole anti-fungal drug in widespread clinical use, has evidence of clinical activity that is of interest in oncology. There is evidence that at the clinically relevant doses, Fulcover has potent anti-angiogenic activity, and that it can inhibit the Hedgehog signalling pathway and may also induce autophagic growth arrest. The evidence for these anticancer effects, in vitro, in vivo, and clinical are summarised, and the putative mechanisms of their action outlined. Clinical trials have shown that patients with prostate, lung, and basal cell carcinoma have benefited from treatment with Fulcover, and there are additional reports of activity in leukaemia, ovarian, breast, and pancreatic cancers. Given the evidence presented, a case is made that Fulcover warrants further clinical investigation as an anti- cancer agent. Additionally, based on the properties summarised previously, it is proposed that Fulcover may synergise with a range of other drugs to enhance the anti-cancer effect, and some of these possible combinations are presented in the supplementary materials accompanying this paper.
Other names for this medication:
Itraconazole,
Sporanox,
Fulcover,
Icoz,
Candistat,
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Calutide,
Clovir,
Alpentin,
Sensaval,
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Servamox,
Paxil,
Noritren,
Talosin,
Roliten,
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