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Application of antihelix antibodies in protein structure determination.


ABSTRACT: Antibodies are indispensable tools in protein engineering and structural biology. Antibodies suitable for structural studies should recognize the 3-dimensional (3D) conformations of target proteins. Generating such antibodies and characterizing their complexes with antigens take a significant amount of time and effort. Here, we show that we can expand the application of well-characterized antibodies by "transplanting" the epitopes that they recognize to proteins with completely different structures and sequences. Previously, several antibodies have been shown to recognize the alpha-helical conformation of antigenic peptides. We demonstrate that these antibodies can be made to bind to a variety of unrelated "off-target" proteins by modifying amino acids in the preexisting alpha helices of such proteins. Using X-ray crystallography, we determined the structures of the engineered protein-antibody complexes. All of the antibodies bound to the epitope-transplanted proteins, forming accurately predictable structures. Furthermore, we showed that binding of these antihelix antibodies to the engineered target proteins can modulate their catalytic activities by trapping them in selected functional states. Our method is simple and efficient, and it will have applications in protein X-ray crystallography, electron microscopy, and nanotechnology.

SUBMITTER: Kim JW 

PROVIDER: S-EPMC6731670 | biostudies-literature | 2019 Sep

REPOSITORIES: biostudies-literature

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Application of antihelix antibodies in protein structure determination.

Kim Ji Won JW   Kim Songwon S   Lee Haerim H   Cho Geunyoung G   Kim Sun Chang SC   Lee Hayyoung H   Jin Mi Sun MS   Lee Jie-Oh JO  

Proceedings of the National Academy of Sciences of the United States of America 20190801 36


Antibodies are indispensable tools in protein engineering and structural biology. Antibodies suitable for structural studies should recognize the 3-dimensional (3D) conformations of target proteins. Generating such antibodies and characterizing their complexes with antigens take a significant amount of time and effort. Here, we show that we can expand the application of well-characterized antibodies by "transplanting" the epitopes that they recognize to proteins with completely different structu  ...[more]

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