The fingerprints of the host innate immunity on the cells of primary virus-induced tumors

As shown earlier, the cells transformed in vitro by various oncogenes, during subsequent in vivo growth were gradually replaced by descendant tumor cells, which co-expressed highly increased H 2O 2-catabolizing antioxidant activity (H 2O 2 CA), and the ability to release PGE 2 (PGE S) in contact wit...

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Bibliographic Details
Published in:Immunology letters 2001-01, Vol.75 (3), p.209-214
Main Authors: Deichman, Galina, Dyakova, Natalya, Kashkina, Lidia, Matveeva, Valentina, Uvarova, Elvira
Format: Article
Language:English
Subjects:
Adenoviruses, Simian - pathogenicity
Adenoviruses, Simian - physiology
Animals
Avian Sarcoma Viruses - pathogenicity
Avian Sarcoma Viruses - physiology
Cell antioxidant activity
Cell Transformation, Viral
Cricetinae
Hydrogen Peroxide - metabolism
Immunity, Innate
Innate host antitumor immunity
Killer Cells, Natural - immunology
Macrophages - immunology
Mesocricetus
Mph
Neoplasms - immunology
Neoplasms - pathology
Neoplasms - virology
Neoplasms, Unknown Primary
NK cells
PGE 2 secretion
Phenotype
Primary viral carcinogenesis
Prostaglandins E - metabolism
Rous sarcoma virus
Simian virus 40
Simian virus 40 - pathogenicity
Simian virus 40 - physiology
Tumor Cells, Cultured
v-srg gene
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Summary:As shown earlier, the cells transformed in vitro by various oncogenes, during subsequent in vivo growth were gradually replaced by descendant tumor cells, which co-expressed highly increased H 2O 2-catabolizing antioxidant activity (H 2O 2 CA), and the ability to release PGE 2 (PGE S) in contact with natural killer cells; v-src was the only oncogene, which in vitro induced cells transformation characterised with the expression of [H 2O 2 CA+PGE S] phenotype. Expression of [H 2O 2 CA+PGE S] phenotype was providing tumor cells with significantly increased resistance to cytotoxic activities of macrophages and NK cells. However, the possible involvement of [H 2O 2 CA+PGE S] phenotype in primary carcinogenesis remained obscure. Here, using three models of the primary virus-induced Syrian hamster tumors we demonstrated that Rous Sarcoma Virus-induced tumors arising after short latent period expressed [H 2O 2 CA + PGE S] phenotype at appearance. During the latent periods of SV40- and SA7(C8)-induced tumors the cells expressing [H 2O 2 CA+PGE S] phenotype gradually replaced the original [H 2O 2 CA+PGE S]-phenotype-negative cell populations. The effectiveness of such selection correlated with the duration of in vivo tumor development. Thus it was shown, that selection of tumor cells expressing [H 2O 2 CA+PGE S] phenotype is beginning and may be completed during the latent period of primary carcinogenesis. Taken together, data of this and preceding our studies on [H 2O 2 CA+PGE S] phenotype demonstrate that in vivo the host innate immunity antitumor reactions are apparently responsible for the selection of rare tumor cell variants capable to defend themselves against CTA of Mph and NK.
ISSN:0165-2478
1879-0542
DOI:10.1016/S0165-2478(00)00304-7