Schistosoma haematobium extracellular vesicle proteins confer protection in a heterologous model of schistosomiasis

Journal Publication ResearchOnline@JCU
Mekonnen, Gebeyaw G.;Tedla, Bemnet A.;Pickering, Darren;Becker, Luke;Wang, Lei;Zhan, Bin;Bottazzi, Maria Elena;Loukas, Alex;Sotillo, Javier;Pearson, Mark S.
Abstract

Helminth parasites release extracellular vesicles which interact with the surrounding host tissues, mediating host–parasite communication and other fundamental processes of parasitism. As such, vesicle proteins present attractive targets for the development of novel intervention strategies to control these parasites and the diseases they cause. Herein, we describe the first proteomic analysis by LC-MS/MS of two types of extracellular vesicles (exosome-like, 120k pellet vesicles and microvesicle-like, 15k pellet vesicles) from adult Schistosoma haematobium worms. A total of 57 and 330 proteins were identified in the 120k pellet vesicles and larger 15k pellet vesicles, respectively, and some of the most abundant molecules included homologues of known helminth vaccine and diagnostic candidates such as Sm-TSP2, Sm23, glutathione S-transferase, saponins and aminopeptidases. Tetraspanins were highly represented in the analysis and found in both vesicle types. Vaccination of mice with recombinant versions of three of these tetraspanins induced protection in a heterologous challenge (S. mansoni) model of infection, resulting in significant reductions (averaged across two independent trials) in liver (47%, 38% and 41%) and intestinal (47%, 45% and 41%) egg burdens. These findings offer insight into the mechanisms by which anti-tetraspanin antibodies confer protection and highlight the potential that extracellular vesicle surface proteins offer as anti-helminth vaccines.

Journal

Vaccines

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Volume

8

ISBN/ISSN

2076-393X

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Issue

3

Pages Count

19

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Publisher

MDPI

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DOI

10.3390/vaccines8030416