Functional and molecular characterization of interleukin‐2 transgenic Ewing tumor cells for in vivo immunotherapy
- 8 April 2004
- journal article
- research article
- Published by Wiley in Pediatric Blood & Cancer
- Vol. 43 (1) , 23-34
- https://doi.org/10.1002/pbc.20013
Abstract
Background Interleukin‐2 (IL‐2) is a potent cytokine with potential activity against several tumors including Ewing tumors (ET). Side effects of systemic IL‐2 can be circumvented by the use of transgenic tumor cells. However, in vitro manipulation may change the overall gene expression profile of tumor cells unfavorably. Therefore, we assessed gene expression profiles, safety, and immunomodulatory efficacy of IL‐2 transgenic (IL‐2‐tg) ET cells in vitro and in NOD/scid mice. Procedure Viable wild type A673 tumor cells were co‐cultured together with irradiated IL‐2‐tg or mock‐transfected cells and HLA matched peripheral blood mononuclear cells. Activation of T and NK cells was assessed by FACS analysis. The effect of irradiated IL‐2‐tg cells on tumor growth in vivo was investigated by using NOD/scid mice. Gene expression profiles of wild type and transfected cells were analyzed with Affymetrix HG‐U95A microarrays. Results IL‐2‐tg cells activated and in creased the number of T cells and NK cells in vitro. Co‐culture with IL‐2‐tg but not with mock‐transfected cells almost completely suppressed wild type tumor cell growth in vitro. Cell depletion experiments indicated a major contribution of NK cells to this tumor cell suppression. Co‐transfer of irradiated IL‐2‐tg cells significantly reduced wild type tumor growth in NOD/scid mice. Side effects in the treated animals were not observed and no tumor growth was observed after injection of irradiated IL‐2‐tg cells alone. Gene expression profiling revealed a substantial degree of homogeneity of gene expression in transfected and wild type cells and suggests that transfection and selection procedures had no major impact on the gene expression profile. Conclusions Next to a high degree of homogeneity between transgenic and wild type cells, our data suggest that irradiated IL‐2‐tg ET cells can activate cytolytic effector cells. These cells may have therapeutic potential for ET patients.Keywords
This publication has 49 references indexed in Scilit:
- Local and systemic effects of an allogeneic tumor cell vaccine combining transgenic human lymphotactin with interleukin-2 in patients with advanced or refractory neuroblastomaBlood, 2003
- IFNγ sensitizes for apoptosis by upregulating caspase-8 expression through the Stat1 pathwayOncogene, 2002
- Regression of tumors by IFN-α electroporation gene therapy and analysis of the responsible genes by cDNA arrayGene Therapy, 2002
- SECRETED TYPE OF MODIFIED INTERLEUKIN-18 GENE TRANSDUCED INTO MOUSE RENAL CELL CARCINOMA CELLS INDUCES SYSTEMIC TUMOR IMMUNITYJournal of Urology, 2001
- Significance analysis of microarrays applied to the ionizing radiation responseProceedings of the National Academy of Sciences, 2001
- Systematic variation in gene expression patterns in human cancer cell linesNature Genetics, 2000
- Interleukin-2 Gene-Modified Allogeneic Tumor Cells for Treatment of Relapsed NeuroblastomaHuman Gene Therapy, 1998
- lnterleukin-2 programs mouse αβ T lymphocytes for apoptosisNature, 1991
- A Progress Report on the Treatment of 157 Patients with Advanced Cancer Using Lymphokine-Activated Killer Cells and Interleukin-2 or High-Dose Interleukin-2 AloneNew England Journal of Medicine, 1987
- Constant-Infusion Recombinant Interleukin-2 in Adoptive Immunotherapy of Advanced CancerNew England Journal of Medicine, 1987