ROLE OF NEUTROPHILS AND CD4+ LYMPHOCYTES-T IN THE PRIMARY AND MEMORY RESPONSE TO NONIMMUNOGENIC MURINE MAMMARY ADENOCARCINOMA MADE IMMUNOGENIC BY IL-2 GENE

被引:0
|
作者
CAVALLO, F
GIOVARELLI, M
GULINO, A
VACCA, A
STOPPACCIARO, A
MODESTI, A
FORNI, G
机构
[1] UNIV ROME LA SAPIENZA, DEPT HUMAN BIOPATHOL, I-00185 ROME, ITALY
[2] UNIV LAQUILA, DEPT EXPTL MED, I-67100 LAQUILA, ITALY
[3] UNIV CHIETI, UER EXPTL PATHOL, CHIETI, ITALY
[4] UNIV TURIN, INST MICROBIOL, I-10124 TURIN, ITALY
来源
JOURNAL OF IMMUNOLOGY | 1992年 / 149卷 / 11期
关键词
D O I
暂无
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
TS/A is a spontaneous adenocarcinoma, apparently not immunogenic in BALB/cnAnCr mice. TS/A cells are unable to stimulate a syngeneic antitumor response either in vitro or in vivo. To evaluate the immunogenic potential of IL-2-releasing neoplastic cells, we used an expression vector to introduce the cDNA coding for murine IL-2 into TS/A cells. Six clones releasing between 30 and 6800 U of IL-2/10(5) cells/ml/48 h have been isolated. Both low (30 U, B1.30) and high (6000 U, B4.6000) IL-2-releasing clone are capable of stimulating a proliferative and cytotoxic response in syngeneic cultures. While the B1.30 clone grows in 60% of syngeneic mice with a delayed pattern, the five clones that release higher levels of IL-2 are promptly rejected. Rejection is associated with neutrophil infiltration, the intensity of which is directly proportional to the amount of IL-2 released. NK cells and CD4+ lymphocytes are uninfluential, whereas CD8+ lymphocytes play only a minor role. This neutrophil-dominated rejection leaves a long-lasting, tumor-specific, T lymphocyte-mediated immune memory. For its induction, CD4+ lymphocytes are required. Their specific activation appears to depend on both the amount of IL-2 released and the granulocyte-mediated reaction that may lead to a more efficient presentation of tumor-associated Ag. These data support the notion that, after transduction of IL-2 gene, cancer cells may elicit an immune antitumor response, and stress the potential use of IL-2 as a component of new tumor vaccines.
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页码:3627 / 3635
页数:9
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