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	Induction of the immune response against HPV16-associated tumours with experimental vaccines Kalenská, Romana ; Reiniš, Milan (advisor) ; Krulová, Magdaléna (referee) 5 Induction of the immune response against HPV16-associated tumours with experimental vaccines The E6/E7 oncoproteins of human papillomaviruses are expressed in most trans- formed cells of cervical carcinoma and, therefore, are attractive targets for T cell-mediated immunotherapy. We have investigated the capacity of vaccines based on E7 oncoprotein- derived peptides to induce cellular immune responses and their therapeutic potential for treatment of minimal residual disease after surgery in a murine experimental model mi- micking human HPV16-associated carcinomas. We compared the effect of E749-57 peptide (RAHYNIVTF) exhibiting immunodominant epitope recognized by cytotoxic T lymphocy- tes with E744-62 peptide (QAEPDRAHYNIVTFCCKCD = 8Q) exhibiting CTL, TH and B- cell epitopes. Immune responses were compared in healthy mice and in mice after surgery or chemotherapy of tumours with ifosfamide derivative CBM-4A. Cellular immune re- sponses were monitored in spleen cells of C57BL/6 mice using ELISPOT-IFN-γ and 51 Cr- release assay. Flow cytometry was used for the detection of CD4+ , CD8+ , CD4+ CD25+ , Gr-1+ CD11b+ and CD3+ NK1.1+ populations. Vaccination with 8Q peptide and synthetic CpG oligodeoxynucleotide as adjuvant induced stronger antitumour immune responses than immunodominant CTL epitope alone in both... Detailed record
	Dendritic cells and their role in the regulation of the immune system Kalenská, Romana ; Frič, Jan (advisor) ; Krulová, Magdaléna (referee) Detailed record
	Induction of the immune response against HPV16-associated tumours with experimental vaccines Kalenská, Romana ; Krulová, Magdaléna (referee) ; Reiniš, Milan (advisor) 5 Induction of the immune response against HPV16-associated tumours with experimental vaccines The E6/E7 oncoproteins of human papillomaviruses are expressed in most trans- formed cells of cervical carcinoma and, therefore, are attractive targets for T cell-mediated immunotherapy. We have investigated the capacity of vaccines based on E7 oncoprotein- derived peptides to induce cellular immune responses and their therapeutic potential for treatment of minimal residual disease after surgery in a murine experimental model mi- micking human HPV16-associated carcinomas. We compared the effect of E749-57 peptide (RAHYNIVTF) exhibiting immunodominant epitope recognized by cytotoxic T lymphocy- tes with E744-62 peptide (QAEPDRAHYNIVTFCCKCD = 8Q) exhibiting CTL, TH and B- cell epitopes. Immune responses were compared in healthy mice and in mice after surgery or chemotherapy of tumours with ifosfamide derivative CBM-4A. Cellular immune re- sponses were monitored in spleen cells of C57BL/6 mice using ELISPOT-IFN-γ and 51 Cr- release assay. Flow cytometry was used for the detection of CD4+ , CD8+ , CD4+ CD25+ , Gr-1+ CD11b+ and CD3+ NK1.1+ populations. Vaccination with 8Q peptide and synthetic CpG oligodeoxynucleotide as adjuvant induced stronger antitumour immune responses than immunodominant CTL epitope alone in both... Detailed record

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