Folia Biologica
Journal of Cellular and Molecular Biology, Charles University 

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Fol. Biol. 2005, 51, 12-18

https://doi.org/10.14712/fb2005051010012

Characteristic of Two Mouse bcr-abl-Transformed Cell Lines: I. General Properties of the Cells

E. Sobotková1, V. Ludvíková1, M. Petráčková1, M. Dušková1, K. Smetana2, F. Jelínek1, I. Marinov3, Vladimír Vonka1

1Department of Experimental Virology, Institute of Hematology and Blood Transfusion, Prague, Czech Republic
2Clinical Department, Institute of Hematology and Blood Transfusion, Prague, Czech Republic
3Laboratory of Flow Cytometry, Institute of Hematology and Blood Transfusion, Prague, Czech Republic

Received January 2005
Accepted January 2005

In an effort to develop an experimental system suitable for immunological studies in which BcrAbl-positive cells are to be used as antigens, we examined the properties of two mouse (Balb/c) established cell lines that express the Bcr-Abl protein and are oncogenic for syngeneic animals. Under standard conditions the two cell lines, viz. Ba-p210 (B210) and 12B1, expressed comparable amounts of the Bcr-Abl protein. However, they differed in a number of characteristics. From the morphological point of view, B210 cells were the more homogeneous, being mainly represented by leukaemic blastic cells with a large number of AgNORs as markers indicating a high proliferative activity. 12B1 cells were more polymorphic and giant cells were detected within their populations. Many 12B1 cells exhibited nuclear segmentation and “band-like“ structures. Markers of proliferation were less frequent in 12B1 and the tendency for aging was more pronounced in these cells. The 12B1 cells were slightly more sensitive to imatinib mesylate than B210 cells. In B210 cells, the expression of MHC class I was downregulated, which was not the case with 12B1 cells. Both cell lines induced leukaemia-like disease in mice after intravenous application but, as compared with B210, 12B1 cells were about 100 times more oncogenic and the disease they induced was more aggressive. Moreover, 12B1, but not B210, induced tumours after subcutaneous or intraperitoneal inoculation.

Funding

The research work was supported by the Grant Agency of the Ministry of Health, Czech Republic, grant No. NC/6957–3.

References

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