BSP Spring Meeting 2024
Schedule : Back to Carolina De Marco Verissimo
Poster
35

Heterogeneous glycosylation of proteins from Fasciola hepatica invasive stage reveals higher complexity in parasite-host interactions

Authors

C De Marco Verissimo2; K Cwiklinski1; J Nilsson3; E Mirgorodskaya3; C Jin3; NG Karlsson4; JP Dalton21 Institute of Infection, Veterinary and Ecological Sciences, University of Liverpool, UK;  2 Centre for One Health and Ryan Institute. University of Galway, Ireland;  3 Proteomics Core Facility, Sahlgrenska Academy of Science, University of Gothenburg, Gothenburg, Sweden;  4 Department of Life Science and Health, Faculty of Health Science, Oslo Metropolitan University, Oslo, Norway

Discussion

Fasciola hepatica is a parasitic trematode that uses glycosylated excreted-secreted (ES) and surface molecules to interact with host cells and tissues, and to evade damage caused by cellular and immune responses during host invasion. Despite the unknown glycosylation state of many of the ~100 different proteins found in the ES of the immature invasive stage of F. hepatica (NEJs), several are extensively used as diagnostic and vaccine targets. To develop more effective strategies against fascioliasis, information on the glycosylation profile of individual NEJs proteins is critical. In this study, we used a combination of glycan, glycopeptide, and proteomic analyses, along with bioinformatics tools, to identify the glycosylation status of individual F. hepatica NEJs proteins. Our results identified 123 glycoproteins in NEJs extracts, 71 of which were in the ES. We mapped 367 glycopeptides and all the 1,696 N-glycan forms and 37 O-glycan forms to their respective protein and glycosites, revealing a high degree of heterogeneity in the glycosylation of F. hepatica NEJs proteins (i.e., in average, 14 different glycan forms can be used to modify each glycoprotein). Unique glycan motifs, such as PC and multi-PC terminals, and xylosylated O-glycan cores, were found in 25 distinct NEJs glycoproteins, including cathepsin peptidases B and L, which are well-known vaccine and diagnostic targets. Furthermore, many parasite proteins carried highly truncated N-glycans and structures with undefined linkages that could not be assigned (i.e., HexNAc2Hex4dHex1), and the roles of which in parasite infection are largely unknown. These structures modify glycoproteins that are excreted-secreted or predicted to be membrane-bound, suggesting that they play key roles in NEJs interactions that command host invasion. Our findings demonstrate that F. hepatica NEJs generate great protein variability via glycosylation, and highlight that the larvae extracts are far more complex than anticipated by proteomic analysis. This data provides a foundation for improving diagnostics and vaccine development to control fascioliasis. 

Hosted By

British Society for Parasitology (BSP)

We are science based Charitable Incorporated Organisation

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