J.Jpn. Surg. Soc.. 95(9): 678-688, 1994
Original article
EFFECT OF LAK CELLS AND BRM ON THE GROWTH OF PANCREATIC CANCER CELLS INJECTED INTO NUDE MICE
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First Department of Surgery, Tohoku University, School of Medicine, Sendai, Japan Haruhiko Asano, Masao Kobari, Tohru Yusa, Kazutake Kawakami, Seiki Matsuno |
Human rIL-2 stimulated spleen cells from BALB/c nu/nu mice were used as effector LAK cells. Human pancreatic cancer cell lines PK-1 and PK-9 were used as target for cytolytic activities against pancreatic cancer. Cytolysis was estimated by 51Cr release assay in vitro, and tumor growth inhibition was estimated by Winn assay in vivo. NK, LAK and pancreatic cancer cell killing activities of LAK cells were elevated to significantly high level of 82%, 70% 51% (PK-1) and 33% (PK-9) respectively on the 2nd day after cultivation with rlL-2. Significantly high level of tumor inhibition rate (98%) was obtained when PK-1 cells were injected into nude mice subcutaneously with LAK cells compared with injection of PK-1 cells only (control). Spleen cells induced from nude mice injected intraperitoneally with rIL-2 or OK- 432 showed significantly high cytolytic activities. These results indicate that LAK cells induced by in vitro or in vivo stimulation with BRM could inhibit the growth of pancreatic cancer.
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