Osteopontin induces increased invasiveness and plasminogen activator expression of human mammary epithelial cells

被引:0
|
作者
Alan B Tuck
Denise M Arsenault
Frances P O'Malley
Charulata Hota
Michael C Ling
Sylvia M Wilson
Ann F Chambers
机构
[1] London Health Sciences Centre,Department of Pathology
[2] University of Western Ontario,Department of Oncology
[3] London Health Sciences Centre,Department of Surgery
[4] University of Western Ontario,undefined
[5] London Health Sciences Centre,undefined
[6] University of Western Ontario,undefined
[7] London Regional Cancer Centre,undefined
来源
Oncogene | 1999年 / 18卷
关键词
osteopontin (OPN); invasion; plasminogen activator; urokinase; mammary epithelial cells; breast cancer;
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中图分类号
学科分类号
摘要
Osteopontin (OPN) has been associated with enhanced malignancy in breast cancer, but its functional role in this disease is poorly understood. To study the effect of OPN on cellular invasiveness, basal OPN expression was first assessed in members of a progression series of human mammary epithelial cell lines (21PT: immortalized, non-tumorigenic; 21NT: weakly tumorigenic; 21MT-1: tumorigenic, weakly metastatic; MDA-MB-435 cells: tumorigenic, highly metastatic). The two lines which expressed lowest basal levels of OPN (21PT, 21NT) were then examined for up-regulation of invasive behavior in response to exogenous or transfected (endogenous) OPN. Both 21PT and 21NT showed increased invasiveness through Matrigel when human recombinant (hr)OPN was added to the lower chamber of transwells. Both also showed a cell migration response to hrOPN. Populations of 21PT and 21NT cells stably transfected with an OPN-expression vector showed higher levels of cell invasiness than control vector transfectants. Examination of transfectants for mRNA of a number of secreted proteases showed that only urokinase-type plasminogen activator (uPA) expression was closely associated with OPN expression and cellular invasiveness. Treatment of the parental 21PT and 21NT cells with exogenous hrOPN resulted in increased uPA mRNA expression and increased urokinase activity of the conditioned media. Both increased cell migration and induction of uPA expression are thus potential mechanisms of increased invasiness of breast epithelial cells in response to OPN.
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页码:4237 / 4246
页数:9
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