Internal Cleavages of the Autoinhibitory Prodomain Are Required for Membrane Type 1 Matrix Metalloproteinase Activation,although Furin Cleavage Alone Generates Inactive Proteinase |
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| Authors: | Vladislav S. Golubkov Piotr Cieplak Alexei V. Chekanov Boris I. Ratnikov Alexander E. Aleshin Natalya V. Golubkova Tatiana I. Postnova Ilian A. Radichev Dmitri V. Rozanov Wenhong Zhu Khatereh Motamedchaboki Alex Y. Strongin |
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| Affiliation: | From the Cancer Research Center, Sanford-Burnham Medical Research Institute, La Jolla, California 92037 |
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| Abstract: | The functional activity of invasion-promoting membrane type 1 matrix metalloproteinase (MT1-MMP) is elevated in cancer. This elevated activity promotes cancer cell migration, invasion, and metastasis. MT1-MMP is synthesized as a zymogen, the latency of which is maintained by its prodomain. Excision by furin was considered sufficient for the prodomain release and MT1-MMP activation. We determined, however, that the full-length intact prodomain released by furin alone is a potent autoinhibitor of MT1-MMP. Additional MMP cleavages within the prodomain sequence are required to release the MT1-MMP enzyme activity. Using mutagenesis of the prodomain sequence and mass spectrometry analysis of the prodomain fragments, we demonstrated that the intradomain cleavage of the PGD↓L50 site initiates the MT1-MMP activation, whereas the 108RRKR111↓Y112 cleavage by furin completes the removal and the degradation of the autoinhibitory prodomain and the liberation of the functional activity of the emerging enzyme of MT1-MMP. |
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| Keywords: | Breast Cancer Matrix Metalloproteinase Protein Degradation Protein Folding Protein Secretion Serine Protease MT1-MMP Furin Prodomain Proteolysis |
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