Literature DB >> 22113774

Novel high-affinity binders of human interferon gamma derived from albumin-binding domain of protein G.

Jawid N Ahmad1, Jingjing Li, Lada Biedermannová, Milan Kuchař, Hana Sípová, Alena Semerádtová, Jiří Cerný, Hana Petroková, Pavel Mikulecký, Jiří Polínek, Ondřej Staněk, Jiří Vondrášek, Jiří Homola, Jan Malý, Radim Osička, Peter Sebo, Petr Malý.   

Abstract

Recombinant ligands derived from small protein scaffolds show promise as robust research and diagnostic reagents and next generation protein therapeutics. Here, we derived high-affinity binders of human interferon gamma (hIFNγ) from the three helix bundle scaffold of the albumin-binding domain (ABD) of protein G from Streptococcus G148. Computational interaction energy mapping, solvent accessibility assessment, and in silico alanine scanning identified 11 residues from the albumin-binding surface of ABD as suitable for randomization. A corresponding combinatorial ABD scaffold library was synthesized and screened for hIFNγ binders using in vitro ribosome display selection, to yield recombinant ligands that exhibited K(d) values for hIFNγ from 0.2 to 10 nM. Molecular modeling, computational docking onto hIFNγ, and in vitro competition for hIFNγ binding revealed that four of the best ABD-derived ligands shared a common binding surface on hIFNγ, which differed from the site of human IFNγ receptor 1 binding. Thus, these hIFNγ ligands provide a proof of concept for design of novel recombinant binding proteins derived from the ABD scaffold.
Copyright © 2011 Wiley Periodicals, Inc.

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Year:  2011        PMID: 22113774     DOI: 10.1002/prot.23234

Source DB:  PubMed          Journal:  Proteins        ISSN: 0887-3585


  15 in total

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