Abstract
Schistosomiasis, caused by parasitic helminths, remains a serious human disease in the tropics. Cercariae of Schistosoma mansoni infect their hosts by direct skin penetration, aided by secretions from acetabular and head glands. Both proteolytic and immunomodulatory properties have been ascribed to the released material, but to date only five isoforms of elastase and one putative anti-inflammatory protein (Sm16) have been cloned. We analyzed secretions from mechanically transformed cercariae by two-dimensional electrophoresis. An average gel image was created and compared with a separation of soluble larval extract, revealing a less complex spot pattern in the secretions with 60% of the spots matched to the larval extract. Subsequent tandem mass spectrometric analysis identified 48 spots from the released material, representing approximately 80% of its normalized volume. Twenty-nine of these are likely to originate in the vesicles, and 18 are likely to originate in the cytosol of the glands (the latter class being present due to holocrine secretion); one is unknown. The vesicular proteins were significantly more enriched than the cytosolic proteins in the released material when compared with the larval extract. A novel metalloproteinase (termed SmPepM8) was the second most abundant constituent after three isoforms of cercarial elastase. In addition, a dipeptidyl peptidase IV (SmDPP IV) was discovered but in much smaller quantity. A new serine protease inhibitor (SmSerp_c) was also prominent. Along with Sm16, four potential immunomodulators were identified, three with similarity to venom allergens (SmSCP_a, _b, and _c) and one with homology to the potassium channel blockers in scorpion venom (SmKK7). Interrogation of the expressed sequence tag database found transcripts encoding the majority of vesicular proteins present solely in the intramolluscan stages of the life cycle. Distinct patterns of radiolabel incorporation suggested three separate origins for the vesicular proteins. All the novel constituents merit investigation as vaccine candidates, and the potential immunomodulators merit investigation as therapeutic agents.
Highlights
Schistosomiasis, caused by parasitic helminths, remains a serious human disease in the tropics
The eggs pass to the gut lumen and continue the life cycle or travel downstream to lodge in the liver where they initiate the pathology that is the hallmark of the disease
The vesicular proteins accounted for 54% of the normalized spot volume with two proteases alone, SmCE and SmPepM8, comprising 34.4 and 12.8% normalized volume (NV), respectively
Summary
Processing of Cercariae and Their Secretions—A Puerto Rican isolate of S. mansoni was maintained by routine passage through albino Biomphalaria glabrata snails and MF1 outbred mice. The medium was removed and centrifuged at 130 ϫ g at 4 °C for 8 min, and the supernatant was stored at Ϫ20 °C with the addition of 20 l of 20ϫ general use protease inhibitor mixture (Sigma). This soluble preparation, termed the 0 –3-h released proteins (RPs), was filter-concentrated to ϳ1 ml using a 5-kDa-molecular mass cutoff Ultrafree-15 unit (Millipore, Watford, UK), and protein content was assayed using Coomassie Plus 200 reagent (Perbio, Tattenhall, Cheshire, UK). A SYPRO Ruby-stained SCAP gel containing 200 g of protein was subjected to software analysis and matched to the average 0 –3-h RP image to enable the -fold difference
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