AI Article Synopsis
- During early schistosomiasis infection, juvenile Schistosoma blood flukes utilize immune system signals to aid their development.
- Researchers found that the S. mansoni cysteine protease SmCB1 triggers a specific IgE immune response before the presence of schistosome eggs.
- This IgE response relies on CD4+ T cell help and IL-4, indicating that type 2 immune responses are activated during early infection stages, and humans exposed to the parasite also produce IgE against SmCB1.
Article Abstract
Background: During the pre-patent stage of infection, juvenile Schistosoma blood flukes co-opt signals from the adaptive immune system to facilitate parasite development, but the types of responses that are induced at this early stage of infection, and the parasite antigens they target, have not been characterized.
Results: Through analysis of experimental pre-patent infections, we show that the S. mansoni cysteine protease SmCB1 is rapidly targeted by an antigen-specific IgE response. The induction of this response is independent of schistosome eggs as infection with male or female worms alone also induced SmCB1-specific IgE. We also show that the SmCB1-specific IgE response is dependent on cognate CD4+ T cell help and IL-4, suggesting that pre-patent Th2 responses provide T cell help for the SmCB1-specific IgE response. Finally, exposed human subjects also produced IgE against SmCB1.
Conclusions: Our data demonstrate that, like eggs, schistosome worms also induce functional type 2 responses and that a parasite cysteine protease is an inducer of type 2 responses during the early stages of schistosome infection.
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|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2993659 | PMC |
| http://dx.doi.org/10.1186/1471-2172-11-56 | DOI Listing |
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