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Synthetic antibody libraries focused towards peptide ligands.

J Mol Biol.. 2008-05;  378(3):622-33
Cobaugh CW, Almagro JC, Pogson M, Iverson B, Georgiou G. 1 Institute for Cell and Molecular Biology, University of Texas at Austin, 2500 Speedway MBB 3.312, Austin, TX 78712, USA2 Centocor R&D, Inc., 145 King of Prussia Road, Office R3621, Radnor, PA 19087, USA3 Department of Chemistry and Biochemistry, University of Texas at Austin, Campus Mail Code A5300, Austin, TX 78712, USA4 Department of Chemical Engineering, University of Texas at Austin, Austin, TX 78712, USA
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摘要

Synthetic antibody libraries have proven immensely useful for the de novo isolation of antibodies without the need for animal immunization. Recently, focused libraries designed to recognize particular classes of ligands, such as haptens or proteins, have been employed to facilitate the selection of high-affinity antibodies. Focused libraries are built using V regions encoding combinations of canonical structures that resemble the structural features of antibodies that bind the desired class of ligands and sequence diversity is introduced at residues typically involved in recognition. Here we describe the generation and experimental validation of two different single-chain antibody variable fragment libraries th... More

关键词

immunoglobulins; hypervariable loops; framework; complementarity-determining regions; canonical structures