Library of binding protein scaffolds (LibBP): a computational platform for selection of binding protein scaffolds
Motivation: Developments in biotechnology have enabled the in vitro evolution of binding proteins. The emerging limitations of antibodies in binding protein engineering have led to suggestions for other proteins as alternative binding protein scaffolds. Most of these proteins were selected based on human intuition rather than systematic analysis of the available data. To improve this strategy, we developed a computational framework for finding desirable binding protein scaffolds by utilizing protein structure and sequence information. Results: For each protein, its structure and the sequences of evolutionarily-related proteins were analyzed, and spatially contiguous regions composed of highly variable residues were identified. A large number of proteins have these regions, but leucine rich repeats (LRRs), histidine kinase domains and immunoglobulin domains are predominant among them. The candidates suggested as new binding protein scaffolds include histidine kinase, LRR, titin and pentapeptide repeat protein
- Publisher
- OXFORD UNIV PRESS
- Issue Date
- 2016-06
- Language
- English
- Article Type
- Article
- Keywords
LEUCINE-RICH REPEAT; DISPLAY; ARCHITECTURE; RECOGNITION; SURFACES; DESIGN; MOTIF
- Citation
BIOINFORMATICS, v.32, no.11, pp.1709 - 1715
- ISSN
- 1367-4803
- Appears in Collection
- BiS-Journal Papers(저널논문)
- Files in This Item
- There are no files associated with this item.
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