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Enhanced susceptibility of target KMT-17 cells to activated macrophages by treatment with the antitumor agent bleomycin
Authors:Zhen-Yi Xu  Masuo Hosokawa  Kiyoshi Morikawa  Hiroshi Kobayashi
Institution:(1) Laboratory of Pathology, Cancer Institute, Hokkaido University School of Medicine, 060 Sapporo, Japan;(2) Present address: Laboratory of Immunology, Cancer Institute, Harbin Medical College, China
Abstract:Summary We observed that after KMT-17 cells had been treated with bleomycin (BLM), even with a dose as high as 160 mgrg/ml, they were still able to form colonies in soft agar. We then studied the susceptibility of KMT-17 cells treated with BLM to activated macrophages. During a colony inhibition assay, BLM-treated KMT-17 cells were found to be much more susceptile to activated macrophages than nontreated KMT-17 cells, moreover, a tumor neutralizing assay showed that the growth of BLM-treated KMT-17 cells was also significantly inhibited by activated macrophages as compared with nontreated KMT-17 cells. Macrophages activated by both BLM and the Nocardia rubra cell wall skeleton were able to mediate such tumor inhibition activity in BLM-treated KMT-17 cells. Activated macrophages did not seem to have strong antitumor activity against nontreated KMT-17 cells in vivo, however, the life span of the rats which were inoculated i. p. with KMT-17 cells was significantly expanded after the tumorbearing rats were given BLM i.p. The data presented here suggest that not only does BLM have a direct tumoricidal effect on KMT-17 cells, it also regulates immunosensitivity of targets to immune effectors. We also discuss the mechanism for enhancing the susceptibility of KMT-17 cells to activated macrophages brought about by treatment with BLM.Supported in part by a Grant-in-Aid for Cancer Research from the Japanese Ministry of Education, Science, and Culture
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