Pleiotrophic Inhibition of Pericellular Urokinase-type Plasminogen Activator System by Endogenous Tumor Suppressive Maspin

Biochemistry and Biophysics

Pleiotrophic Inhibition of Pericellular Urokinase-type Plasminogen Activator System by Endogenous Tumor Suppressive Maspin¹

Hector Biliran, Jr. and Shijie Sheng²

Department of Pathology, Wayne State University School of Medicine, Detroit, Michigan 48201

Maspin is a novel serine protease inhibitor with tumor suppressiveactivity, inhibiting tumor invasion and metastasis. To date,the underlying molecular mechanism of maspin remains elusive.Recombinant maspin has been shown to specifically inhibit cellsurface-associated urokinase-type plasminogen activator (uPA)and fibrinogen-bound tissue-type plasminogen activator. However,the role of endogenous maspin in plasminogen activation is totallyunknown. To address this issue, we generated stable maspin-expressingtransfectants using prostate carcinoma cells DU145 as the parentalcell line. We report here that endogenous maspin exerts pleiotropicinhibitory effects on the pericellular uPA system. Maspin expressionled to a significantly reduced level of cell surface-bound uPAand uPA receptor proteins without altering the steady-statelevels of the respective mRNAs. Treatment with receptor-associatedprotein (RAP), a specific inhibitor of low-density lipoproteinreceptor-related protein, lead to a significantly increasedlevel of secreted uPA and cell surface uPAR in maspin transfectantsbut not in the mock control cells. A combination of enzymaticand molecular analyses revealed that maspin inhibits the cellsurface-mediated plasminogen activation by forming an SDS-resistantcomplex with cell surface-bound uPA. In addition, maspin expressionled to a dramatic reduction in the release of active uPA, bothhigh molecular weight and the low molecular weight, into theconditioned culture medium. Consistently, the conditioned mediumof maspin transfectant clones had a significantly reduced activityin converting plasminogen to plasmin. The inhibitory effectof maspin on pericellular uPA correlates with significantlydecreased cell invasion potential and motility in vitro. Themaspin-neutralizing antibody (Abs4A) reversed the subdued invasivepotential of maspin transfectant cells in a dose-dependent manner.In summary, this study provides the first evidence that endogenousmaspin is a potent inhibitor of pericellular uPA. Furthermore,our results support a current hypothesis that maspin blockstumor invasion and motility by inhibiting localized pericellularproteolysis.

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