Inhibition of cell proliferation in HCC-9204 hepatoma cells by a c-myc specific ribozyme

被引:0
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作者
Jin Cheng
Jinyan Luo
Xueyong Zhang
Jialu Hu
Hongxiang Hui
Chengji Wang
Arnold Stern
机构
[1] New York University Medical Center,Department of Pharmacology
[2] Institute of Gastroenterology,Department of Biochemistry and Molecular
[3] The Second College of Xian Medical University,Biology
[4] Institute of Gastroenterology,undefined
[5] The Xijing Hospital of The Fourth Military Medical University,undefined
[6] The Fourth Military Medical University,undefined
来源
Cancer Gene Therapy | 2000年 / 7卷
关键词
Hepatoma cells; ribozyme; c-; retroviral vector.;
D O I
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中图分类号
学科分类号
摘要
A ribozyme (RZ) gene targeting c-myc mRNA was synthesized and cloned. Cleavage reaction showed that cleavage of the RZ was efficient and specific. The RZ gene-containing retrovirus vector pDOR-RZ was transfected into HCC-9204 hepatoma cells, which constitutively express high levels of c-myc using Lipofectamine. Positively transfected cells were selected using G418. In situ hybridization showed that both pDOR-RZ and pDOR vectors had been integrated into the chromosome of HCC-9204 cells. Dot blot hybridization indicated that expression of the RZ was only evident in pDOR-RZ-transfected HCC-9204 cells. Avidin-biotin complex enzyme-linked immunosorbent assay showed that c-myc expression was down-regulated. Chromatin aggregation into compact masses, cytoplasmic vacuole degeneration, and blurring of cytoplasm structure were observed by transmission electron microscopy in HCC-9204-RZ cells. These results suggest that the use of a c-myc mRNA cleaving enzyme could be most effective in tumor cells that are highly proliferative and constitutively express high levels of c-myc.
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页码:407 / 412
页数:5
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