IL-2 gene therapy of solid tumors: An approach for the prevention of signal transduction defects in T cells Journal Article


Authors: Zier, K. S.; Gansbacher, B.
Article Title: IL-2 gene therapy of solid tumors: An approach for the prevention of signal transduction defects in T cells
Abstract: The identification of tumor-associated antigens has focused attention on the mechanisms that underlie the failure of T cells to destroy tumor cells. A deeper understanding of the process of signal transduction following the binding of ligand by the T cell receptor can help to identify underlying defects that may be involved. Gene therapy using tumor cells genetically modified to express cytokines or surface determinants is a promising technique for stimulating antitumor responses. A potential pitfall in its application to cancer, however, is that some patients' T cells are immune suppressed and may resist stimulation by such genetically engineered vaccines. Recent studies have demonstrated that T cells from tumor-bearing patients exhibit abnormalities in signal transduction events, possibly rendering them unable to respond to activation signals. Gene therapy with interleukin 2 secreting tumor cells in an animal model has been shown effective in preventing the onset of signaling defects. A more precise definition of the molecular mechanisms that enable cytokine-secreting tumor cells to stimulate specific antitumor responses may make it feasible to optimize immunotherapeutic approaches resulting in better clinical results.
Keywords: signal transduction; review; nonhuman; neoplasms; t cells; t lymphocyte; t-lymphocytes; animals; mice; interleukin 2; animal experiment; tumor cell; gene therapy; forecasting; tumor immunity; immunosuppressive treatment; interleukin-2; immune suppression; humans; human
Journal Title: Journal of Molecular Medicine
Volume: 74
Issue: 3
ISSN: 0946-2716
Publisher: Springer  
Date Published: 1996-03-01
Start Page: 127
End Page: 134
Language: English
DOI: 10.1007/bf01575444
PUBMED: 8846162
PROVIDER: scopus
DOI/URL:
Notes: Source: Scopus
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