Mapping of the conserved antigenic domains shared between potato apyrase and parasite ATP diphosphohydrolases: potential application in human parasitic diseases

Author:

FARIA-PINTO P.,REZENDE-SOARES F. A.,MOLICA A. M.,MONTESANO M. A.,MARQUES M. J.,ROCHA M. O. C.,GOMES J. A. S.,ENK M. J.,CORREA-OLIVEIRA R.,COELHO P. M. Z.,NETO S. M.,FRANCO O. L.,VASCONCELOS E. G.

Abstract

SUMMARYEvolutionary and closer structural relationships are demonstrated by phylogenetic analysis, peptide prediction and molecular modelling betweenSolanum tuberosumapyrase,Schistosoma mansoniSmATPase 2 andLeishmania braziliensisNDPase. Specific protein domains are suggested to be potentially involved in the immune response, and also seem to be conserved during host and parasite co-evolution. Significant IgG antibody reactivity was observed in sera from patients with American cutaneous leishmaniasis (ACL) and schistosomiasis using potato apyrase as antigen in ELISA.S. mansoniadult worm or egg,L. braziliensispromastigote (Lb) andTrypanosoma cruziepimastigote (EPI) have ATP diphosphohydrolases, and antigenic preparations of them were evaluated. In ACL patients, IgG seropositivity was about 43% and 90% for Lb and potato apyrase, respectively, while IgM was lower (<19%) for both. In schistosomiasis patients IgM (>40%) or IgG (100%) seropositivity for both soluble egg (SEA) and adult worm (SWAP) antigens was higher than that found for potato apyrase (IgM=10%; IgG=39%). In Chagas disease, IgG seropositivity for EPI and potato apyrase was 97% and 17%, respectively, while the IgM was low (3%) for both antigens. The study of the conserved domains from both parasite proteins and potato apyrase could lead to the development of new drug targets or molecular markers.

Publisher

Cambridge University Press (CUP)

Subject

Infectious Diseases,Animal Science and Zoology,Parasitology

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