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01121 Journal of Nara Medical Association >
Vol.54 No.5-6 >
このアイテムの引用には次の識別子を使用してください:
http://hdl.handle.net/10564/211
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タイトル: | 多剤耐性遺伝子(MDR1)過剰発現肝細胞癌に対するelectrochemotherapyの有用性に関する基礎的検討 |
その他のタイトル: | ELECTROCHEMOTHERAPY CAN OVERCOME P-LYCOPROTEIN RELATED TUMOR RESISTANCE IN HEPATOCELLULAR CARCINOMA |
著者: | 西脇, 功 |
キーワード: | electrochemotherapy multidrug resistance gene 1 hepatocellular carcinoma adriamycin |
発行日: | 2003年12月31日 |
出版者: | 奈良医学会 奈良県立医科大学 |
引用: | Journal of Nara Medical Association Vol.54 No.5-6 p.293-303 |
抄録: | The aim of this study was to investigate the role of electroporation in the
treatment of carcinoma expressing multidrug resistance gene 1 (MDR1). The cells stably
expressing MDR1 gene (BNL/MDR1-Bulk) and the clone expressing the MDR1 gene at
the highest level (BNL/MDR1-Clone) were established by transducing human MDR1
gene into the mouse hepatocellular carcinoma (HCC) cell line, BNLIME.7R.1. The
expressions of P-glycoprotein on the cell surface of the established HCC cells,
BNL/MDR1-Bulk and BNL/MDR1-Clone, were determined by fluorescence-activated cell
sorter (FACS) with the monoclonal antibody MRK16, specific against human
P-glycoprotein. BNL/MDR1-Bulk expressed P-glycoprotein on the cell surface at various
levels, and BNL/MDR1-Clone expressed it at the highest level. In vitro, BNL/MDR1-Bulk
and BNL/MDR1-Clone exhibited approximately 8-fold and 10-fold higher resistance
against adriamycin, respectively, 4-fold and 10-fold higher resistance against vinblastin,
respectively, and 2-fold and 5-fold higher resistance against mitomycin C, respectively.
When these cells were exposed to adriamycin with electroporation in vitro, the
chemosensitivities against adriamnycin were increased, reaching the level of the parental
cells (BNL/Wild). In the mouse models of subcutaneous tumors produced by inoculation
of these cells, electroporation alone or injection of adriamycin at 1/10 of the 50% lethal
dosage could not inhibit the growth of the tumor. However, electrochemotherapy
consisting of adriamycin injection with electroporation did inhibit tumor growth not
only in mice inoculated with the parental HCC cells or BNL/Wild cells, but also in
P-glycoprotein presenting mice inoculated with BNL/MDR1-Bulk or BNL/MDR1-Clone.
These results indicated that electrochemotherapy has the potential to overcome the tumor
resistance related to MDR function in hepatoma cells. |
URI: | http://hdl.handle.net/10564/211 |
ISSN: | 13450069 |
出現コレクション: | Vol.54 No.5-6
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