| کد مقاله | کد نشریه | سال انتشار | مقاله انگلیسی | نسخه تمام متن |
|---|---|---|---|---|
| 2144903 | 1548027 | 2011 | 9 صفحه PDF | دانلود رایگان |
Cellular activation of latent matrix metalloproteinase-2 (proMMP-2) requires formation of a cell membrane-associated activation complex that involves specific binding between the hemopexin domain of proMMP-2 (PEX) and the C-terminal domain of tissue inhibitor of matrix metalloproteinases-2 (C-TIMP-2). In this study, we tested the feasibility of inhibiting activation of proMMP-2 by exogenous inhibitors, which block the binding between PEX and TIMP-2. The recombinant C-TIMP-2 and synthetic peptides from C-TIMP-2 were used as inhibitors for proMMP-2 activation. Recombinant C-TIMP-2 bound specifically to both the catalytically inactive MMP-2E404A and the C-terminal domain of MMP-2 (PEX) in a concentration dependent manner with apparent Kd of 3.9 × 10−7 M and 1.7 × 10−7 M, respectively. Moreover, C-TIMP-2 competed the binding between MMP-2E404A and full-length TIMP-2. Finally, activity assays showed that addition of C-TIMP-2 to HT-1080 fibrosarcoma cells inhibited proMMP-2 activation in a concentration-dependent manner. We then designed a synthetic peptide, P175L, consisting of 20 residues from the PEX-binding tail region of C-TIMP-2. P175L bound PEX and inhibited cell membrane-mediated activation of proMMP-2 in a concentration dependent manner. Deletion of the last 9 tail residues of C-TIMP-2 in P175L abrogated the inhibitory activities of the peptide showing that these residues were essential for function. Overall, these experiments have demonstrated that proMMP-2 activation can be inhibited by exogenous inhibitors which points to a potential strategy for MMP-2 specific inhibition.
► Inhibition of activation of proMMP-2 by peptides was investigated.
► Isolated C-terminal domain of TIMP-2 bound and inhibited activation of proMMP-2.
► A 20-residue peptide from the tail of C-TIMP-2 inhibited activation of proMMP2.
► The last 9 residues of C-TIMP-2 are essential for TIMP-2 interactions with proMMP-2.
Journal: Matrix Biology - Volume 30, Issues 7–8, September–October 2011, Pages 404–412