Identification and immunological characterization of three potential vaccinogens against Cryptosporidium species
Fecha
2011Autor
Patricio A. Manque [Chile. Universidad Mayor. Centro de Genómica y Bioinformatica]
Tenjo, Fernando [Virginia Commonwealth University. Center for the Study of Biological Complexity]
Woehlbier, Ute [Virginia Commonwealth University. Center for the Study of Biological Complexity]
Lara, Ana M. [Virginia Commonwealth University. Center for the Study of Biological Complexity]
Serrano, Myrna G. [Virginia Commonwealth University. Center for the Study of Biological Complexity]
Xu, Ping [Virginia Commonwealth University. Center for the Study of Biological Complexity]
Alves, Joao MP. [Virginia Commonwealth University. Center for the Study of Biological Complexity]
Smeltz, Ronald B. [Virginia Commonwealth University. Center for the Study of Biological Complexity]
Conrad, Daniel H. [Virginia Commonwealth University. Center for the Study of Biological Complexity]
Buck, Gregory A. [Virginia Commonwealth University. Center for the Study of Biological Complexity]
Ubicación geográfica
Notas
HERRAMIENTAS
Resumen
Cryptosporidiosis is a ubiquitous infectious disease, caused by the protozoan parasites Cryptosporidium hominis and Cryptosporidium parvum, leading to acute, persistent, and chronic diarrhea with life-threatening consequences in immunocompromised individuals. In developing countries, cryptosporidiosis in early childhood has been associated with subsequent significant impairment in growth, physical fitness, and intellectual abilities. Currently, vaccines are unavailable and chemotherapeutics are toxic and impractical, and agents for immunoprophylaxis or treatment of cryptosporidiosis are a high priority. Availability of the genome sequences for C. hominis and C. parvum provides new opportunities to procure and examine novel vaccine candidates. Using the novel approach of “reverse vaccinology,” we identified several new potential vaccine candidates. Three of these antigens—Cp15, profilin, and a Cryptosporidium apyrase—were delivered in heterologous prime-boost regimens as fusions with cytolysin A (ClyA) in a Salmonella live vaccine vector and as purified recombinant antigens, and they were found to induce specific and potent humoral and cellular immune responses, suggesting their potential as new vaccinogens against Cryptosporidium infection.
URI
http://repositorio.umayor.cl/xmlui/handle/sibum/2556https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3209039/pdf/zcd1796.pdf
https://dx.doi.org/10.1128/CVI.05197-11
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