Author:
COCUDE C.,PIERROT C.,CÊTRE C.,FONTAINE J.,GODIN C.,CAPRON A.,KHALIFE J.
Abstract
The isolation of 2 genomic clones has allowed us to further characterize
a Schistosoma mansoni serine protease designated
SmSP1. The deduced amino acid sequence (248aa) considered as a ‘light
chain’ encoding the active site, presents
significant homologies with mouse plasma kallikrein and human factor I
light chain. The secondary structure of SmSP1
‘light chain’ is correctly predicted and may be sufficient
by itself to constitute an active enzyme. The biological function
of SmSP1 is unknown, however, the homology with 2 serine proteases suggests
that SmSP1 may play a role in the evasion
of the host immune response. This is supported by the presence of the native
protein corresponding to SmSP1 particularly
in schistosomula released products (SRP) and in male dorsal spines. The
expression of this enzyme is differentially
regulated throughout the parasite life-cycle. However, infected animals
with S. mansoni did not produce specific antibodies
to recombinant SmSP1. The lack of such response could be advantageous to
the parasite by protecting itself from host
effector mechanisms.
Publisher
Cambridge University Press (CUP)
Subject
Infectious Diseases,Animal Science and Zoology,Parasitology
Cited by
15 articles.
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