Aminopeptidase N1 (EtAPN1), an M1 Metalloprotease of the Apicomplexan Parasite Eimeria tenella, Participates in Parasite Development
Author(s) -
Simon Gras,
Anna Byzia,
Florence B. Gilbert,
Sheena McGowan,
Marcin Drąg,
Anne Silvestre,
Alisson Niepceron,
Fabien Lecaille,
Gilles Lalmanach,
Fabien Brossier
Publication year - 2014
Publication title -
eukaryotic cell
Language(s) - English
Resource type - Journals
eISSN - 1535-9778
pISSN - 1535-9786
DOI - 10.1128/ec.00062-14
Subject(s) - biology , eimeria , aminopeptidase , plasmodium falciparum , parasite hosting , metalloproteinase , apicomplexa , leucyl aminopeptidase , biochemistry , plasmodium (life cycle) , microbiology and biotechnology , enzyme , leucine , amino acid , malaria , immunology , world wide web , computer science
Aminopeptidases N are metalloproteases of the M1 family that have been reported in numerous apicomplexan parasites, includingPlasmodium ,Toxoplasma ,Cryptosporidium , andEimeria . While investigating the potency of aminopeptidases as therapeutic targets against coccidiosis, one of the most important avian diseases caused by the genusEimeria , we identified and characterizedEimeria tenella aminopeptidase N1 (EtAPN1). Its inhibition by bestatin and amastatin, as well as its reactivation by divalent ions, is typical of zinc-dependent metalloproteases. EtAPN1 shared a similar sequence, three-dimensional structure, and substrate specificity and similar kinetic parameters with A-M1 fromPlasmodium falciparum (PfA-M1), a validated target in the treatment of malaria. EtAPN1 is synthesized as a 120-kDa precursor and cleaved into 96-, 68-, and 38-kDa forms during sporulation. Further, immunolocalization assays revealed that, similar to PfA-M1, EtAPN1 is present during the intracellular life cycle stages in both the parasite cytoplasm and the parasite nucleus. The present results support the hypothesis of a conserved role between the two aminopeptidases, and we suggest that EtAPN1 might be a valuable target for anticoccidiosis drugs.
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