Abstract
BackgroundSchistosomes are able to survive for prolonged periods in the blood system, despite continuous contact with coagulatory factors and mediators of the host immune system. Protease inhibitors likely play a critical role in host immune modulation thereby promoting parasite survival in this extremely hostile environment. Even though Kunitz type serine protease inhibitors have been shown to play important physiological functions in a range of organisms these proteins are less well characterised in parasitic helminths.MethodsWe have cloned one gene sequence from S. mansoni, Smp_147730 (SmKI-1) which is coded for single domain Kunitz type protease inhibitor, E. coli-expressed and purified. Immunolocalisation and western blotting was carried out using affinity purified polyclonal anti-SmKI-1 murine antibodies to determine SmKI-1 expression in the parasite. Protease inhibitor assays and coagulation assays were performed to evaluate the functional roles of SmKI-1.ResultsSmKI-1 is localised in the tegument of adult worms and the sub-shell region of eggs. Furthermore, this Kunitz protein is secreted into the host in the ES products of the adult worm. Recombinant SmKI-1 inhibited mammalian trypsin, chymotrypsin, neutrophil elastase, FXa and plasma kallikrein with IC50 values of 35 nM, 61 nM, 56 nM, 142 nM and 112 nM, respectively. However, no inhibition was detected for pancreatic elastase or cathepsin G. SmKI-1 (4 μM) delayed blood clot formation, reflected in an approximately three fold increase in activated partial thromboplastin time and prothrombin time.ConclusionsWe have functionally characterised the first Kunitz type protease inhibitor (SmKI-1) from S. mansoni and show that it has anti-inflammatory and anti-coagulant properties. SmKI-1 is one of a number of putative Kunitz proteins in schistosomes that have presumably evolved as an adaptation to protect these parasites from the defence mechanisms of their mammalian hosts. As such they may represent novel vaccine candidates and/or drug targets for schistosomiasis control.Electronic supplementary materialThe online version of this article (doi:10.1186/s13071-015-1022-z) contains supplementary material, which is available to authorized users.
Highlights
Schistosomes are able to survive for prolonged periods in the blood system, despite continuous contact with coagulatory factors and mediators of the host immune system
Analyses of SmKI-1 Sequence searches revealed the presence of seven putative Kunitz proteins in S. mansoni (Additional file 1)
Clustal alignment (Fig. 1) of the Kunitz domains of these putative S. mansoni Kunitz proteins and bovine pancreatic trypsin inhibitor (BPTI) showed that the amino acid sequence is highly conserved within the domain
Summary
Schistosomes are able to survive for prolonged periods in the blood system, despite continuous contact with coagulatory factors and mediators of the host immune system. Despite constant contact with immune components in the human blood system, adult schistosome worms are capable of surviving for prolonged periods in the mesenteric veins of humans, in some instances, more than 30 years, without triggering host inflammatory reactions or promoting thrombus (blood clot) formation [1]. S. mansoni prolonged activated partial thromboplastin time (APTT) and was able to block the enzymatic activation of factor XI (plasma thromboplastin antecedent; PTA) by factor Xlla (activated Hageman factor) [2] but the precise molecule(s) involved have not been identified. It is, likely that schistosome protease inhibitors play a role in interacting with the proteases involved in blood coagulation. It has been suggested that studies on protease inhibitors can advance the understanding of host-parasite biology and lead to the identification of novel vaccine candidates and/or drug targets against schistosomes [6]
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