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A 45-Amino-Acid Scaffold Mined from the PDB for High-Affinity Ligand Engineering.


ABSTRACT: Small protein ligands can provide superior physiological distribution compared with antibodies, and improved stability, production, and specific conjugation. Systematic evaluation of the PDB identified a scaffold to push the limits of small size and robust evolution of stable, high-affinity ligands: 45-residue T7 phage gene 2 protein (Gp2) contains an ? helix opposite a ? sheet with two adjacent loops amenable to mutation. De novo ligand discovery from 10(8) mutants and directed evolution toward four targets yielded target-specific binders with affinities as strong as 200 ± 100 pM, Tms from 65 °C ± 3 °C to 80°C ± 1 °C, and retained activity after thermal denaturation. For cancer targeting, a Gp2 domain for epidermal growth factor receptor was evolved with 18 ± 8 nM affinity, receptor-specific binding, and high thermal stability with refolding. The efficiency of evolving new binding function and the size, affinity, specificity, and stability of evolved domains render Gp2 a uniquely effective ligand scaffold.

SUBMITTER: Kruziki MA 

PROVIDER: S-EPMC4536934 | biostudies-literature | 2015 Jul

REPOSITORIES: biostudies-literature

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A 45-Amino-Acid Scaffold Mined from the PDB for High-Affinity Ligand Engineering.

Kruziki Max A MA   Bhatnagar Sumit S   Woldring Daniel R DR   Duong Vandon T VT   Hackel Benjamin J BJ  

Chemistry & biology 20150709 7


Small protein ligands can provide superior physiological distribution compared with antibodies, and improved stability, production, and specific conjugation. Systematic evaluation of the PDB identified a scaffold to push the limits of small size and robust evolution of stable, high-affinity ligands: 45-residue T7 phage gene 2 protein (Gp2) contains an α helix opposite a β sheet with two adjacent loops amenable to mutation. De novo ligand discovery from 10(8) mutants and directed evolution toward  ...[more]

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