Adenovirus vaccination againstneu oncogene exerts long-term protection from tumorigenesis in BALB/neuT transgenic mice
| Autor: | Guido Forni, Barbara Cipriani, Maurizio Nuzzo, Paolo Monaci, Pasquale Gallo, Daniele Maldini, Sridhar Dharmapuri |
|---|---|
| Rok vydání: | 2006 |
| Předmět: |
Genetically modified mouse
Cancer Research Time Factors Receptor ErbB-2 Genetic Vectors Molecular Sequence Data Epitopes T-Lymphocyte Mice Transgenic Spleen medicine.disease_cause Injections Intramuscular Adenoviridae Cell Line Mice Mammary Glands Animal Immune system Cell Line Tumor Proliferating Cell Nuclear Antigen medicine Animals Humans Amino Acid Sequence Codon Mice Inbred BALB C biology Vaccination Mammary Neoplasms Experimental Molecular biology Rats Gene Expression Regulation Neoplastic medicine.anatomical_structure Oncology Tumor progression Immunology NIH 3T3 Cells biology.protein Female Antibody Intramuscular injection Carcinogenesis |
| Zdroj: | International Journal of Cancer. 120:574-584 |
| ISSN: | 1097-0215 0020-7136 |
| DOI: | 10.1002/ijc.22274 |
| Popis: | The transforming rat HER2/neu oncogene (neu), when embedded in the genome of transgenic BALB/c (neuT) mice, provokes the development of an invasive carcinoma in each of their 10 mammary glands. We used the neuT mice model system to evaluate the immunization efficiency and the protective effect of intramuscular injection of adenovirus (Ad) and/or of DNA with electrostimulation (DNA+ES), both expressing the rat p185neu protein. A neu cDNA sequence, which exclusively contains codons preferred by highly expressed mammalian genes, was used in this study. This “optimized” cDNA displayed higher expression in cultured cells and greater cell-mediated response than the original gene when injected as DNA+ES. Ad expressing the optimized sequence (Ad5-neu.opt) induced a higher immune response, as measured by the frequency of IFN-γ-secreting spleen cells and antibody titers. Different Ad/DNA combinations and immunization schedules confirmed the superiority of Ad5-neu.opt in inducing a strong Th1-skewed humoral and CD8+ cell-mediated response. Two Ad5-neu.opt injections of 109 viral particles at week 10 and 12 were sufficient to induce the highest response, which persisted at detectable levels up to 33 weeks of age. Anti-Ad5 antibodies elicited by previous injections neutralized the effect of an additional Ad5-neu.opt immunization at week 19. A group, which received 3 injections of DNA+ES at week 23, 27 and 31, in addition to the 3 Ad injections at week 10, 12 and 19 showed an increased frequency of IFN-γ+, CD8+ PBMC at week 25, which persisted at detectable levels till week 38. Ad5-neu.opt administration at 10 and 12 weeks of age had a significant impact on tumor progression. At 44 weeks, 40% of the mice were completely protected from tumors with a mean tumor of 3.8. In contrast, control mice developed 10 tumors and died by week 27. Vaccination blocked the tumor development at the atypical hyperplasia stage present at the time of treatment. Tumors developing at later times express reduced levels of rat p185neu protein. © 2006 Wiley-Liss, Inc. |
| Databáze: | OpenAIRE |
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