Insights into the mechanism of anti-tumor immunity in mice vaccinated with the human HER2/ neu extracellular domain plus anti-HER2/ neu IgG3-(IL-2) or anti-HER2/ neu IgG3-(GM-CSF) fusion protein

In the present study, we demonstrate that a physical association between the extracellular domain of human HER2/ neu receptor (ECD HER2) plus anti-HER2/ neu IgG3-(IL-2) or anti-HER2/ neu IgG3-(GM-CSF) was required to elicit the most effective anti-tumor immune response against a syngeneic tumor expr...

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Veröffentlicht in:Vaccine 2005-09, Vol.23 (39), p.4793-4803
Hauptverfasser: Dela Cruz, Jay S., Morrison, Sherie L., Penichet, Manuel L.
Format: Artikel
Sprache:eng
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Zusammenfassung:In the present study, we demonstrate that a physical association between the extracellular domain of human HER2/ neu receptor (ECD HER2) plus anti-HER2/ neu IgG3-(IL-2) or anti-HER2/ neu IgG3-(GM-CSF) was required to elicit the most effective anti-tumor immune response against a syngeneic tumor expressing rat HER2/ neu. Immune effectors including CD4 +, CD8 +, and NK cells contributed to protection against tumor growth. Vaccinated B-cell deficient mice did not elicit tumor protection, suggesting a critical role for B-cells in a protective immune response. These results provide insights into the mechanisms responsible for the protective tumor immunity elicited when antibody-(IL-2 or GM-CSF) are used as enhancers of vaccines targeting tumor antigens.
ISSN:0264-410X
1873-2518
DOI:10.1016/j.vaccine.2005.04.041