Abstract
Schistosomiasis is a parasitic infection caused by Schistosoma flatworms, prime examples of multicellular parasites that live in the mammalian host for many years. Glycoconjugates derived from the parasite have been shown to play an important role in many aspects of schistosomiasis, and some of them are present in the circulation of the host. The aim of this study was to identify novel glycoconjugates related to schistosomiasis in urine of Schistosoma mansoni-infected individuals using a combination of glycopeptide separation techniques and in-depth mass spectrometric analysis. Surprisingly, we characterized a heterogeneous population of novel aberrantly O-glycosylated peptides derived from the C terminus of human apolipoprotein C-III (apoC-III) in urine of S. mansoni-infected individuals that were not detected in urine of non-infected controls. The glycan composition of these glycopeptides is completely different from what has been described previously for apoC-III. Most importantly, they lack sialylation and display a high degree of fucosylation. This study exemplifies the potential of mass spectrometry for the identification and characterization of O-glycopeptides without prior knowledge of either the glycan or the peptide sequence. Furthermore, our results indicate for the first time that as a result of S. mansoni infection the glycosylation of a host protein is altered.
Highlights
Schistosomiasis is a parasitic infection caused by Schistosoma flatworms, prime examples of multicellular parasites that live in the mammalian host for many years
Analysis of Glycopeptides in Urine from S. mansoni-infected Individuals and Non-infected Controls—Urine samples collected from S. mansoni-infected individuals and non-infected controls were subjected to organic precipitation to deplete large proteins
Because we were interested in the analysis of schistosomiasisrelated glycopeptides, we primarily focused on the higher m/z ranges
Summary
Schistosomiasis is a parasitic infection caused by Schistosoma flatworms, prime examples of multicellular parasites that live in the mammalian host for many years. The aim of this study was to identify novel glycoconjugates related to schistosomiasis in urine of Schistosoma mansoni-infected individuals using a combination of glycopeptide separation techniques and indepth mass spectrometric analysis. The female worms deposit hundreds of eggs each day Many of these are transferred to the intestine and excreted with the feces to eventually continue the life cycle, but a significant fraction is trapped in the liver of the host instead. The schistosome-specific multifucosylated glycan epitope recognized by a carbohydratespecific antibody that binds to egg glycoprotein antigens has been characterized [12] This antibody immunocaptured free oligosaccharides containing the same multifucosylated structural elements from urine of Schistosoma-infected individuals [13]. We identified a set of aberrantly O-glycosylated, highly fucosylated peptides from human apolipoprotein C-III in urine from infected individuals but not in that from noninfected individuals
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