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Development of highly immunogenic variants of a rat fibrosarcoma line during in vitro cultivation
Authors:Kenji Yamashina  Tusuneyuki Oikawa  Masaharu Kasai  Masaharu Naiki  Itsuo Chiba  Hiroshi Kobayashi
Institution:(1) Laboratory of Pathology, Cancer Institute, Hokkaido University, 060 Sapporo, Japan;(2) Laboratory of Genetics, Cancer Institute, Hokkaido University, 060 Sapporo, Japan;(3) Department of Internal Medicine, Faculty of Medicine, Hokkaido University, 060 Sapporo, Japan;(4) Department of Biochemistry, Facults of Veterinary Medicine, Hokkaido University, 060 Sapporo, Japan;(5) Present address: Department of Immunology, Michigan Cancer Foundation, 48201 Detroit, MI, USA
Abstract:Summary Rat firosarcoma KMT-17 cells descreased in tumorigenicity when cultured in vitro. Eight clones derived from cultured KMT-17 cell lines (c-KMT-17) were examined for their tumorigenicity, immunosensitivity, and immunogenicity. All the clones were less or nontumorigenic in normal syngeneic rats than KMT-17 cells maintained in vivo. All eight clones produced tumors in rats immuno-suppressed with 600 rad 60Co; differences in degree of tumorigenicity were seen among clones in rats irradiated with 250 rad 60Co. Although immunosensitivity of the eight clones to complement-dependent and cell-mediated cytotoxicity was the same or less than that of KMT-17 cells, al leight clones induced greater transplantation resistance to KMT-17 than KMT-17 itself. Cold target inhibition tests demonstrated new antigens in a highly immunogenic variant in addition to the original tumor associated antigen (TAA). New glycolipids, not observed in KMT-17 cells, were demonstrated in the clones by thin layer chromatography. These results suggest that new antigens appearing during culture of KMT-17 may act as helper antigens for TAA, increasing the immunogenicity and decreasing the tumorigenicity of the cultured cells.This work was partially supported by a Grant-in-Aid for Cancer Research from the Ministry of Education, Science und Culture, Japan.
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