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Trivalent vaccine formulation focused on the prophylactic / therapeutic control of tumors induced by human papillomavirus type 16 (HPV-16) and infection by human immunodeficiency virus (HIV) and human herpes virus (HSV).

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Author(s):
Vinicius Canato Santana
Total Authors: 1
Document type: Master's Dissertation
Press: São Paulo.
Institution: Universidade de São Paulo (USP). Instituto de Ciências Biomédicas (ICB/SDI)
Defense date:
Examining board members:
Luis Carlos de Souza Ferreira; Paulo Lee Ho; Eugenia Costanzi Strauss
Advisor: Luis Carlos de Souza Ferreira
Abstract

The proteins E7 (HPV), p24 (HIV) and gD (HSV) are exclusively expressed by infected cells or tumors and therefore are used as targets for vaccines with therapeutic characteristics. We developed two DNA vaccines capable of expressing these three viral proteins using a bicistronic expression vector based on IRES sequence. The plasmid vaccines, named pIRES I and pIRES II, differ by carrying the genes that encode proteins of HPV-16 E7 and p24 fused to the HIV protein gD of HSV-1 in reverse order. Transfected COS-7 cells expressed the target proteins, as determined by immunofluorescence with specific antibodies for gD, p24 and E7. The vaccines were tested in mice for their ability to generate antibodies and specific CD8+ T cells. We observed that vaccinated animals developed low levels of antibodies against gD, E7 and p24. In contrast, we demonstrate the induction of specific CD8+ T cells for the three antigens. The plasmid vaccines were able to protect mice inoculated with TC-1 tumor cells (which express the E7 protein of HPV-16), although with different levels of protection in prophylactic and therapeutic trials. The formulations were tested for ability to protect animals against challenge with HSV-1 and only one of them generated a protective effect. In conclusion, the results show that vaccines directed to therapeutic control of infections or tumor process associated with HPV, HSV or HIV represents a promising and viable goal. (AU)