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Gene-Engineered T Cells as a Superior Adjuvant Therapy for Metastatic Cancer
Author(s) -
Michael H. Kershaw,
Jacob T. Jackson,
Nicole M. Haynes,
Michele W.L. Teng,
Maria Moeller,
Yoshihiro Hayakawa,
Shayna E.A. Street,
Rachel Cameron,
Jane E. Tanner,
Joseph A. Trapani,
Mark J. Smyth,
Phillip K. Darcy
Publication year - 2004
Publication title -
the journal of immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.737
H-Index - 372
eISSN - 1550-6606
pISSN - 0022-1767
DOI - 10.4049/jimmunol.173.3.2143
Subject(s) - adjuvant , medicine , metastatic breast cancer , breast cancer , doxorubicin , cancer research , immune system , adjuvant therapy , cancer , immunology , oncology , chemotherapy
The major limiting factor in the successful application of adjuvant therapy for metastatic disease is the lack of adjuvant specificity that leads to severe side effects. Reasoning that T cells of the immune system are highly specific, we generated tumor-specific T cells by genetic modification of mouse primary T cells with a chimeric receptor reactive with the human breast cancer-associated Ag erbB-2. These T cells killed breast cancer cells and secreted IFN-gamma in an Ag-specific manner in vitro. We investigated their use against metastatic breast cancer in mice in an adjuvant setting, and compared their effectiveness with the commonly applied adjuvants doxorubicin, 5-fluorouracil, and herceptin. Mice were inoculated orthotopically with the human erbB-2-expressing spontaneously metastatic mouse breast cancer 4T1.2 in mammary tissue, and the primary tumor was surgically removed 8 days later. Significant metastatic disease was demonstrated in lung and liver at the time of surgery on day 8 with increased tumor burden at later time points. T cell adjuvant treatment of day 8 metastatic disease resulted in dramatic increases in survival of mice, and this survival was significantly greater than that afforded by either doxorubicin, 5-fluorouracil, or herceptin.

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