Literature DB >> 18499681

Engineering of a femtomolar affinity binding protein to human serum albumin.

Andreas Jonsson1, Jakob Dogan, Nina Herne, Lars Abrahmsén, Per-Ake Nygren.   

Abstract

We describe the development of a novel serum albumin binding protein showing an extremely high affinity (K(D)) for HSA in the femtomolar range. Using a naturally occurring 46-residue three-helix bundle albumin binding domain (ABD) of nanomolar affinity for HSA as template, 15 residues were targeted for a combinatorial protein engineering strategy to identify variants showing improved HSA affinities. Sequencing of 55 unique phage display-selected clones showed a strong bias for wild-type residues at nine positions, whereas various changes were observed at other positions, including charge shifts. Additionally, a few non-designed substitutions appeared. On the basis of the sequences of 12 variants showing high overall binding affinities and slow dissociation rate kinetics, a set of seven 'second generation' variants were constructed. One variant denoted ABD035 displaying wild-type-like secondary structure content and excellent thermal denaturation/renaturation properties showed an apparent affinity for HSA in the range of 50-500 fM, corresponding to several orders of magnitude improvement compared with the wild-type domain. The ABD035 variant also showed an improved affinity toward serum albumin from a number of other species, and a capture experiment involving human serum indicated that the selectivity for serum albumin had not been compromised from the affinity engineering.

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Year:  2008        PMID: 18499681     DOI: 10.1093/protein/gzn028

Source DB:  PubMed          Journal:  Protein Eng Des Sel        ISSN: 1741-0126            Impact factor:   1.650


  49 in total

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7.  Structure-activity analysis of truncated albumin-binding domains suggests new lead constructs for potential therapeutic delivery.

Authors:  Conan K Wang; Anna S Amiss; Joachim Weidmann; David J Craik
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8.  An engineered affibody molecule with pH-dependent binding to FcRn mediates extended circulatory half-life of a fusion protein.

Authors:  Johan Seijsing; Malin Lindborg; Ingmarie Höidén-Guthenberg; Heiko Bönisch; Elin Guneriusson; Fredrik Y Frejd; Lars Abrahmsén; Caroline Ekblad; John Löfblom; Mathias Uhlén; Torbjörn Gräslund
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9.  Biodistribution of a bispecific single-chain diabody and its half-life extended derivatives.

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10.  A 2-helix small protein labeled with 68Ga for PET imaging of HER2 expression.

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