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Proteomic identification of galectin-11 and -14 ligands from Fasciola hepatica. | LitMetric

Proteomic identification of galectin-11 and -14 ligands from Fasciola hepatica.

Int J Parasitol

Department of Animal, Plant and Soil Science and Centre for AgriBioscience (AgriBio), La Trobe University, Victoria 3086, Australia; Centre for Livestock Interactions with Pathogens (CLiP), La Trobe University, Victoria 3086, Australia. Electronic address:

Published: November 2019

AI Article Synopsis

  • Fasciola hepatica is a parasitic trematode that impacts livestock and humans, causing disease and economic loss, with increasing resistance to current treatments.
  • The study focuses on the interaction of two glycan-binding proteins, LGALS-11 and LGALS-14, with F. hepatica proteins, revealing novel insights into potential vaccine candidates.
  • LGALS-14 identified a larger number of interacting proteins than LGALS-11, including previously tested vaccine candidates, indicating its significance in understanding host-parasite dynamics.

Article Abstract

Fasciola hepatica is a globally distributed zoonotic trematode that causes fasciolosis in livestock, wildlife, ruminants and humans. Fasciolosis causes a significant economic impact on the agricultural sector and affects human health. Due to the increasing prevalence of triclabendazole resistance in F. hepatica, alternative treatment methods are required. Many protein antigens have been trialled as vaccine candidates with low success, however, the tegument of F. hepatica is highly glycosylated and the parasite-derived glycoconjugate molecules have been identified as an important mediator in host-parasite interactions and as prime targets for the host immune system. Galectin-11 (LGALS-11) and galectin-14 (LGALS-14) are two ruminant-specific glycan-binding proteins, showing upregulation in the bile duct of sheep infected with F. hepatica, which are believed to mediate host-parasite interaction and innate immunity against internal parasites. For the first known time, this study presents the ligand profile of whole worm and tegument extracts of F. hepatica that interacted with immobilised LGALS-11 and LGALS-14. LGALS-14 interacted with a total of 255 F. hepatica proteins. The protein which had the greatest interaction was identified as an uncharacterised protein which contained a C-type lectin domain. Many of the other proteins identified were previously trialled vaccine candidates including glutathione S-transferase, paramyosin, cathepsin L, cathepsin B, fatty acid binding protein and leucine aminopeptidase. In comparison to LGALS-14, LGALS-11 interacted with only 49 F. hepatica proteins and it appears to have a much smaller number of binding partners in F. hepatica. This is, to our knowledge, the first time host-specific lectins have been used for the enrichment of F. hepatica glycoproteins and this study has identified a number of glycoproteins that play critical roles in host-parasite interactions which have the potential to be novel vaccine candidates.

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Source
http://dx.doi.org/10.1016/j.ijpara.2019.06.007DOI Listing

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