Functional involvement of src and focal adhesion kinase in a CD99 splice variant-induced motility of human breast cancer cells

被引:0
|
作者
Hyuk-Joon Lee
Eunsook Kim
Bokeun Jee
Jang-Hee Hahn
Kyuyoung Han
Kyeong Cheon Jung
Seong Hoe Park
Hansoo Lee
机构
[1] Kangwon National University,Vascular System Research Center, College of Natural Sciences
来源
Experimental & Molecular Medicine | 2002年 / 34卷
关键词
breast cancer; CD99; focal adhesion kinase; motility; splice variant; src;
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学科分类号
摘要
Earlier report showed that expression of a splice variant of CD99 transmembrane protein increases invasive ability of human breast cancer cells. Cell motility was also significantly enhanced by the CD99 splice variant expression. In an effort to identify the cellular components that mediate a signal transduction pathway triggered by the CD99 splice variant, known signal path inhibitors were examined for their effects on the motility of the CD99 splice variant-transfected MDA-MB-231 breast cancer cells. Phenylarsine oxide, an inhibitor of phosphatase specific for focal adhesion kinase, and PP1, an inhibitor of src kinase family, significantly suppressed motility of the cells. Among different types of src transfectant clones generated, kinase-negative mutant src transfectant cells were 80% less motile than the mock cells transfected with an empty-vector, while v-src and c-src transfectants exhibited cell motility levels at or slightly above the mock transfectant. These results suggest that src and focal adhesion kinase mediate the intracellular signaling pathway of a CD99 splice variant for the induction of motility of human breast cancer cells.
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页码:177 / 183
页数:6
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