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Structure-function studies of an engineered scaffold protein derived from stefin A. I: Development of the SQM variant.

Protein Eng Des Sel.. 2010-05;  23(5):403 - 413
Toni Hoffmann, Lukas Kurt Josef Stadler, Michael Busby, Qifeng Song, Anthony T. Buxton, Simon D. Wagner, Jason J. Davis, and Paul Ko Ferrigno. Section of Experimental Therapeutics, Leeds Institute of Molecular Medicine, St James's University Hospital, Beckett St, Leeds LS97TF, UK.
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摘要

Non-antibody scaffold proteins are used for a range of applications, especially the assessment of protein-protein interactions within human cells. The search for a versatile, robust and biologically neutral scaffold previously led us to design STM (stefin A triple mutant), a scaffold derived from the intracellular protease inhibitor stefin A. Here, we describe five new STM-based scaffold proteins that contain modifications designed to further improve the versatility of our scaffold. In a step-by-step approach, we introduced restriction sites in the STM open reading frame that generated new peptide insertion sites in loop 1, loop 2 and the N-terminus of the scaffold protein. A second restriction site in 'lo... More

关键词

circular dichroism spectroscopy; epitope recognition; peptide aptamer; scaffold protein