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Investigation of Carboxypeptidase, Sphingomyelinase and Alkaline Phosphatase from Schistosoma mansoni as potential vaccine candidates.

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Author(s):
Bogar Omar Araujo Montoya
Total Authors: 1
Document type: Doctoral Thesis
Press: São Paulo.
Institution: Universidade de São Paulo (USP). Instituto de Ciências Biomédicas (ICB/SDI)
Defense date:
Examining board members:
Luciana Cezar de Cerqueira Leite; Sirlei Daffre; Ricardo De Marco; Glaucia Maria Machado Santelli; Carlos Eduardo Winter
Advisor: Luciana Cezar de Cerqueira Leite
Abstract

Schistosomiasis is a major public health problem in tropical areas and neglected by most of the pharmaceutical companies. Three genes were selected from S. mansoni transcriptome to be molecularly characterized and tested as vaccines. The Carboxypeptidase gene showed high transcription levels in cercariae stage and a variable protein expression in intra-host stages. The refolded recombinant protein showed limited activity. The Sphingomyelinase gene showed the highest level of transcriptional activity in the egg stage and the protein is expressed in all stages but 7-day old schistosomula and females. The Alkaline Phosphatase gene showed a high transcriptional activity in cercariae stage with most of the mRNA being translated into protein as soon as it penetrates its definitive host. Immunization of mice with each of the three proteins did not show reduction in worm burden recovery after challenge. These results demonstrate that several characteristics of an antigen are important for it to be considered a good vaccine candidate. (AU)

FAPESP's process: 05/04396-0 - Investigation of Schistosoma mansoni carboxypeptidase and sphingomyelinase as potential vaccine candidates
Grantee:Bogar Omar Araujo Montoya
Support Opportunities: Scholarships in Brazil - Doctorate (Direct)