Treatment with tumor-reactive Fab-IL-2 and Fab-staphylococcal enterotoxin A fusion proteins leads to sustained T cell activation, and long-term survival of mice with established tumors.

Søgaard,M; Ohlsson,L; Kristensson,K; Rosendahl,A; Sjoberg,A; Forsberg,G; Kalland,T; Dohlsten,M

doi:10.3892/ijo.15.5.873

Treatment with tumor-reactive Fab-IL-2 and Fab-staphylococcal enterotoxin A fusion proteins leads to sustained T cell activation, and long-term survival of mice with established tumors.

Authors:
- M Søgaard
- L Ohlsson
- K Kristensson
- A Rosendahl
- A Sjoberg
- G Forsberg
- T Kalland
- M Dohlsten
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Affiliations: Active Biotech Research AB, S-220 07 Lund, Sweden.
Published online on: November 1, 1999 https://doi.org/10.3892/ijo.15.5.873
Pages: 873-955

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Abstract

C215Fab-IL-2 fusion protein, with full IL-2 and antigen binding activity, was produced in E. coli at high level (>50 mg/l). When co-administered with Fab-superantigen fusion protein (C215Fab-SEA) in mice strong and sustained T cell activation was observed. Combination treatment of mice carrying B16 melanoma transfected with C215 antigen was also more efficient than using C215Fab-SEA (p<0.01) or C215Fab-IL-2 alone (p<0.001). In a long-term survival experiment 5/12 mice having received combination treatment 5 days after i.v. inoculation of B16 cells survived >85 days. Improved therapeutic efficacy correlated with increased tumor infiltration by activated CD25+ T cells, indicating a T cell mediated mechanism.