Antioxidant gene expression and function inin vitro-developingSchistosoma mansonimother sporocysts: possible role in self-protection

Abstract

SUMMARY: The ability of the larval forms ofSchistosoma mansonito invade and parasitize their molluscan host,Biomphalaria glabrata, is determined by a multitude of factors. In this study we sought to elucidate the possible mechanisms by which the invading larvae are able to counteract the potentially harmful oxidative environment presented by the host upon initial miracidial infection. This was attempted by examining the gene expression profile of parasite antioxidant enzymes of the linked glutathione-(GSH) thioredoxin (Trx) redox pathway during early intramolluscan larval development. Three such enzymes, the peroxiredoxins (Prx1, Prx2 and Prx3) were examined as to their activity and sites of expression withinS. mansonimiracidia andin vitro-cultured mother sporocysts. Results of these studies demonstrated that the H₂O₂-reducing enzymes Prx1 and 2 are upregulated during early mother sporocyst development compared to miracidia. Immunolocalization studies further indicated that Prx1 and Prx2 proteins are expressed within the apical papillae of miracidia and tegumental syncytium of sporocysts, and are released with parasite excretory-secretory proteins (ESP) duringin vitrolarval transformation. Removal of Prx1 and Prx2 from larval ESP by immunoabsorption significantly reduced the ability of ESP to breakdown exogenous H₂O₂, thereby directly linking ESP Prx proteins with H₂O₂-scavenging activity. Moreover, exposure of live sporocysts to exogenous H₂O₂stimulated an upregulation of Prx1 and 2 gene expression suggesting the involvement of H₂O₂–responsive elements in regulating larval Prx gene expression. These data provide evidence that Prx1 and Prx2 may function in the protection ofS. mansonisporocysts during the early stages of infection.