AI Article Synopsis

  • Glycoproteins from helminth parasites, like the liver fluke (Fasciola hepatica), are important for vaccine development but the understanding of their protein glycosylation is limited.
  • This study identifies genes linked to glycosylation in F. hepatica, revealing 149 genes related to sugar uptake and glycosylation, with significant gene duplication.
  • The liver fluke lacks key enzymes for complex glycan production, suggesting its glycans are structurally simple and laying groundwork for future research into targeted parasite control methods.

Article Abstract

Glycoproteins secreted by helminth parasites are immunogenic and represent appealing components of vaccine preparations. Our poor knowledge of the pathways that mediate protein glycosylation in parasitic flatworms hinders our understanding of how proteins are synthesised and modified, and our ability to target these pathways for parasite control. Here we provide the first detailed description of genes associated with protein glycosylation in a parasitic flatworm, focusing on the genome of the liver fluke (Fasciola hepatica), which is a globally important trematode parasite of humans and their livestock. Using 190 human sequences as search queries against currently available F. hepatica genomes, we identified 149 orthologues with putative roles in sugar uptake or nucleotide sugar synthesis, and an array of glycosyltransferase and glycosidase activities required for protein N- and O-glycosylation. We found appreciable duplication within these orthologues, describing just 87 non-redundant genes when paralogues were excluded. F. hepatica lacks many of the enzymes required to produce complex N- and O-linked glycans, which explains the genomic basis for the structurally simple glycans described by F. hepatica glycomic datasets, and predicts pervasive structural simplicity in the wider glycome. These data provide a foundation for functional genomic interrogation of these pathways with the view towards novel parasite intervention strategies.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6076252PMC
http://dx.doi.org/10.1038/s41598-018-29673-3DOI Listing

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