Infection with Fasciola hepatica (liver flukes) causes fascioliasis in humans and fasciolosis in ruminants. The current strategy for controlling fascioliasis/fasciolosis is predominantly mediated by chemotherapy with triclabendazole (TCBZ). As this flukicide targets newly excysted juveniles (NEJs), immature flukes and mature liver flukes, it's use as the frontline chemotherapy for over four decades has led to widespread drug resistance. New chemotherapeutics are, therefore, urgently required. Here, continuing our studies of flukicidal phytochemicals derived from Hedera helix (common ivy), we investigated the anthelmintic properties of three ivy fruit saponins, including α-hederin (IVL-11), against F. hepatica. During ex vivo culture, IVL-11 was as effective as TCBZ in killing NEJs and immature flukes. However, this saponin acted more quickly than TCBZ when tested against mature flukes. Microscopic examination of IVL-11 treated liver flukes revealed surface integrity breaches, actin disorganisation and cell membrane permeabilisation. Upon in vivo studies, using a novel method to isolate IVL-11 in large quantities from H. helix leaf, oral delivery of IVL-11 (up to 250 mg/kg bodyweight) to Ovis aries (sheep) was found to be safe, well-tolerated and detectable in the liver, peripheral blood, hepatic portal blood and bile. IVL-11 (250 mg/kg bodyweight) treatment of O. aries infected with F. hepatica led to a significant reduction in fluke body sizes as well as a delay and decrease in fecundity during in vivo efficacy studies. Together, our results confirm that IVL-11 exhibits flukicidal characteristics suitable for progression as a renewably obtained, natural product for treating fasciolosis.
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Biomedicine & Pharmacotherapy
University of Dundee
KTH Royal Institute of Technology
Texas Tech University
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