| Literature DB >> 29426058 |
Lucie Raisová Stuchlíková1, Věra Králová2, Kateřina Lněničková1, Tomáš Zárybnický1, Petra Matoušková1, Veronika Hanušová2, Martin Ambrož1, Zdeněk Šubrt3, Lenka Skálová1.
Abstract
Flubendazole (FLU), a benzimidazole anthelmintic drug widely used in veterinary medicine, has been approved for the treatment of gut-residing nematodes in humans. In addition, FLU is now considered a promising anti-cancer agent. Despite this, information about biotransformation of this compound in human is lacking. Moreover, there is no information regarding whether cancer cells are able to metabolize FLU in order to deactivate it. For these reasons, the present study was designed to identify all metabolites of Phase I and Phase II of FLU in human liver and in various cancer cells using ultra high-performance liquid chromatography-tandem mass spectrometry (UHPLC-MS/MS) analysis. Precision-cut human liver slices and 9 cell lines of different origin (breast, colon, oral cavity) were used as in vitro model systems. Our study showed that FLU with a reduced carbonyl group (FLUR) is the only FLU metabolite formed in the human liver. All human cancer cell lines were able to form FLUR. In addition, methylated FLUR was detected in breast cells MCF7 and intestinal SW480 cells. The accumulation of FLU and its reduction to FLUR markedly differed among cells. The extent of FLU reduction was in a good correlation with the detected expression level of carbonyl reductase 1. In most cases, FLU entered in a higher amount and was reduced to a lesser extent in proliferating (metastatic) cells than in differentiated (non-cancerous, non-metastatic) ones. These results support the promising potential of FLU in anti-cancer therapy.Entities:
Keywords: anti-cancer drug; biotransformation; carbonyl reduction; drug-drug; interactions
Year: 2018 PMID: 29426058 DOI: 10.1002/dta.2369
Source DB: PubMed Journal: Drug Test Anal ISSN: 1942-7603 Impact factor: 3.345