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A new prodrug form of Affibody molecules (pro-Affibody) is selectively activated by cancer-associated proteases.

Cell Mol Life Sci.. 2014-10; 
Lisa Sandersjöö, Andreas Jonsson, John Löfblom Division of Protein Technology, School of Biotechnology, KTH Royal Institute of Technology, 106 91, Stockholm, Sweden
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摘要

Affinity proteins have advanced the field of targeted therapeutics due to their generally higher specificity compared to small molecular compounds. However, side effects caused by on-target binding in healthy tissues are still an issue. Here, we design and investigate a prodrug strategy for improving tissue specificity of Affibody molecules in future in vivo studies. The prodrug Affibody (pro-Affibody) against the HER2 receptor was constructed by fusing a HER2-specific Affibody (ZHER2) to an anti-idiotypic Affibody (anti-ZHER2). The linker was engineered to comprise a substrate peptide for the cancer-associated matrix metalloprotease 1 (MMP-1). The hypothesis was that the binding surface of ZHER2 would thereby ... More

关键词

HER2; Bacterial display; Combinatorial protein engineering; Staphylococcal display; Directed evolution; Cell surface display; Flow cytometry; MMP-1