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Clinical and Diagnostic Laboratory Immunology, November 2000, p. 932-939, Vol. 7, No. 6
Section of Molecular Parasitology, Department
of Molecular Cell Biology, Sungkyunkwan University School of
Medicine, Suwon 440-746,1 and Department
of Parasitology, Chung-Ang University College of Medicine, Seoul
156-756,2 Korea
Received 31 March 2000/Returned for modification 30 June
2000/Accepted 14 August 2000
A complete cDNA sequence encoding a 28-kDa cruzipain-like cysteine
protease of adult Paragonimus westermani, termed
Pw28CCP, was isolated from an adult cDNA library. The cDNA contained a single open reading frame of 975 bp encoding 325 amino acids, which
exhibited the structural motif and domain organization
characteristic of cysteine proteases of non-cathepsin Bs
including a hydrophobic signal sequence, an ERFNIN motif, and
essential cysteine residues as well as active sites in the mature
catalytic region. Analysis of its phylogenetic position
revealed that this novel enzyme belonged to the cruzipain-like cysteine
proteases. The sequence of the first 13 amino acids predicted from
the mature domain of Pw28CCP was in accord with that
determined from the native 28-kDa enzyme purified from the adult
worm. Expression of Pw28CCP was observed specifically in juvenile and
adult worms, with a location in the intestinal epithelium, suggesting
that this enzyme could be secreted and involved in
nutrient uptake and immune modulation. The recombinant protein
expressed in Escherichia coli was used to assess
antigenicity by immunoblotting with sera from patients with active
paragonimiasis and from those with other parasitic infections. The
resulting sensitivity of 86.2% (56 of 65 samples) and specificity of
98% (147 of 150 samples) suggest its potential as an antigen for use in immunodiagnosis.
1071-412X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
Structural and Immunological Characteristics of a
28-Kilodalton Cruzipain-Like Cysteine Protease of Paragonimus
westermani Expressed in the Definitive Host Stage

*
Corresponding author. Mailing address: Section of
Molecular Parasitology, Department of Molecular Cell Biology,
Sungkyunkwan University School of Medicine, Suwon 440-746, Korea.
Phone: (82) 31 299 6251. Fax: (82) 31 299 6269. E-mail:
kongy{at}yurim.skku.ac.kr.
Present address: Institute of Malariology, College of Medicine,
Inje University, Pusan 614-735, Korea.
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