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The expression and biological activity of IL-2 receptor on a human pancreas cancer cell line
Authors:Hiroyuki Kawami  Kazuhiro Yoshida  Yoshiyuki Yamaguchi  Toshiaki Saeki  Tetsuya Toge
Institution:(1) Department of Surgery, Research Institute for Nuclear Medicine and Biology, Hiroshima University, 1-2-3 Kasumi-cho, Minami-ku, 734 Hiroshima, Japan
Abstract:To ascertain whether the tumor cells can regulate the host immune systems through the production of the cytokines or their receptors, we examined the expressions of tumor necrosis factoragr (TNFagr), tumor necrosis factor Bgr (TNFBgr), interleukin 2 (IL-2) and interleukin 2 receptor alpha chain (IL-2Ragr) on the human cancer cell lines by Northern blot analysis. We used K562 (leukemia cell line), MCF-7 (breast cancer cell line), LS180, HT29 (colon cancer cell lines), SH101 (gastric cancer cell line) and PH101 (pancreas cancer cell line). Expressions of TNFagr, TNFBgr and IL-2 mRNA were not detected in any of the tumor cell lines. However, 1.4 and 3.5 kilobases of the IL-2Ragr mRNA were expressed in the PH101 cells, but not in the other five cell lines. Furthermore, IL-2Ragr was detected on the cell surface of the PH101 cells by the flow-cytometric analysis with an anti-IL-2Ragr monoclonal antibody. Interestingly, the soluble IL-2Ragr (sIL-2Ragr) was found in the conditioned media obtained from the PH101 cell culture with a sandwich enzyme immunoassay. Moreover, the sIL-2Ragr secreted from the PH101 cells blocked the IL-2 dependent lymphocyte proliferation. These results indicate that the expression of IL-2Ragr on PH101 might suppress the IL-2 induced lymphocyte proliferation.
Keywords:IL-2 receptor expression  cancer cell  immunosuppression
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