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Development of High Affinity and High Specificity Inhibitors of Matrix Metalloproteinase 14 through Computational Design and Directed Evolution.

J. Biol. Chem.. 2017; 
Arkadash Valeria,Yosef Gal,Shirian Jason,Cohen Itay,Horev Yuval,Grossman Moran,Sagi Irit,Radisky Evette S,Shifman Julia M,Papo
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Recombinant Proteins to mutation by Sharabi and colleagues (40), and purchased from GenScript (NJ, USA). Briefly Get A Quote

摘要

Degradation of the extracellular matrices in the human body is controlled by matrix metalloproteinases (MMPs), a family of more than 20 homologous enzymes. Imbalance in MMP activity can result in many diseases, such as arthritis, cardiovascular diseases, neurological disorders, fibrosis, and cancers. Thus, MMPs present attractive targets for drug design and have been a focus for inhibitor design for as long as 3 decades. Yet, to date, all MMP inhibitors have failed in clinical trials because of their broad activity against numerous MMP family members and the serious side effects of the proposed treatment. In this study, we integrated a computational method and a yeast surface display techniq... More

关键词

binding affinity,computational protein design,directed evolution,matrix metalloproteinases,metastasis,protease inhibitor,protein-protein interaction,proteolysis,yeast surface dis