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Enhanced coexpression of YB-1 and DNA topoisomerase II α genes in human colorectal carcinomas

✍ Scribed by Kazunori Shibao; Hiroshi Takano; Yoshifumi Nakayama; Keisuke Okazaki; Naoki Nagata; Hiroto Izumi; Takeshi Uchiumi; Michihiko Kuwano; Kimitoshi Kohno; Hideaki Itoh


Book ID
102649594
Publisher
John Wiley and Sons
Year
1999
Tongue
French
Weight
738 KB
Volume
83
Category
Article
ISSN
0020-7136

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✦ Synopsis


The transcription factor YB-1 is expressed in a wide range of cell types and has been implicated in the regulation of various genes involved in cell proliferation. Nuclear expression of YB-1 is correlated with MDR-1 gene expression in breast cancer and osteosarcoma. In this study, we asked whether YB-1 expression is enhanced in human colorectral carcinoma and if it is associated with the expression of target genes such as MDR-1, DNA topoisomerase II ␣ and PCNA. YB-1, DNA topoisomerase II ␣, PCNA and MDR-1 expression were assessed by Western blotting, Northern blotting and immunohistochemistry in 26 human colorectal carcinomas. The involvement of YB-1 in DNA topoisomerase II ␣ gene expression was examined by transient DNA transfection assays. YB-1 was overexpressed in almost all cancerous lesions in comparison with normal mucosa in surgically resected colorectal carcinomas of 26 patients. YB-1 expression correlated well with both DNA topoisomerase II ␣ and PCNA expression. In contrast, no correlation was observed between YB-1 and MDR-1 expression. We also found that a transient co-transfection with a DNA topoisomerase II ␣ promoter-luciferase plasmid and an antisense YB-1 expression construct resulted in a significant reduction of the promoter activity in KM12C human colon cancer cells. YB-1 may be an excellent proliferation-associated marker and may be a transcription factor regulating DNA topoisomerase II ␣ gene expression in human colorectal carcinoma.


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