Computational Evolution of Threonine-Rich β-Hairpin Peptides Mimicking Specificity and Affinity of Antibodies

[Image: see text] The development of recognition molecules with antibody-like properties is of great value to the biotechnological and bioanalytical communities. The recognition molecules presented here are peptides with a strong tendency to form β-hairpin structures, stabilized by alternate threoni...

Descripción completa

Detalles Bibliográficos
Autores principales: Hu, Hongxia, Kofoed, Christian, Li, Ming, Gonçalves, Juliana Pereira Lopes, Hansen, Jonas, Wolfram, Martin, Hansen, Axel Kornerup, Friis Hansen, Camilla Hartmann, Diness, Frederik, Schoffelen, Sanne, Meldal, Morten
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2019
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6396188/
https://www.ncbi.nlm.nih.gov/pubmed/30834314
http://dx.doi.org/10.1021/acscentsci.8b00614
_version_ 1783399217915494400
author Hu, Hongxia
Kofoed, Christian
Li, Ming
Gonçalves, Juliana Pereira Lopes
Hansen, Jonas
Wolfram, Martin
Hansen, Axel Kornerup
Friis Hansen, Camilla Hartmann
Diness, Frederik
Schoffelen, Sanne
Meldal, Morten
author_facet Hu, Hongxia
Kofoed, Christian
Li, Ming
Gonçalves, Juliana Pereira Lopes
Hansen, Jonas
Wolfram, Martin
Hansen, Axel Kornerup
Friis Hansen, Camilla Hartmann
Diness, Frederik
Schoffelen, Sanne
Meldal, Morten
author_sort Hu, Hongxia
collection PubMed
description [Image: see text] The development of recognition molecules with antibody-like properties is of great value to the biotechnological and bioanalytical communities. The recognition molecules presented here are peptides with a strong tendency to form β-hairpin structures, stabilized by alternate threonines, which are located at one face of the peptide. Amino acids at the other face of the peptide are available for interaction with the target molecule. Using this scaffold, we demonstrate that recognition molecules can efficiently be designed in silico toward four structurally unrelated proteins, GFP, IL-1β, IL-2, and IL-6. On solid support, 10 different antibody-mimetic recognition molecules were synthesized. They displayed high affinity and no cross-reactivity, as observed by fluorescence microscopy. Stabilized variants were readily obtained by incorporation of azido acids and propargylglycine followed by cyclization via the Cu(I)-catalyzed alkyne–azide cycloaddition reaction. As this new class of antibody mimics can be designed toward essentially any protein, the concept is believed to be useful to a wide range of technologies. Here, their use in protein separation and in the detection of proteins in a sandwich-type assay is demonstrated.
format Online
Article
Text
id pubmed-6396188
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher American Chemical Society
record_format MEDLINE/PubMed
spelling pubmed-63961882019-03-04 Computational Evolution of Threonine-Rich β-Hairpin Peptides Mimicking Specificity and Affinity of Antibodies Hu, Hongxia Kofoed, Christian Li, Ming Gonçalves, Juliana Pereira Lopes Hansen, Jonas Wolfram, Martin Hansen, Axel Kornerup Friis Hansen, Camilla Hartmann Diness, Frederik Schoffelen, Sanne Meldal, Morten ACS Cent Sci [Image: see text] The development of recognition molecules with antibody-like properties is of great value to the biotechnological and bioanalytical communities. The recognition molecules presented here are peptides with a strong tendency to form β-hairpin structures, stabilized by alternate threonines, which are located at one face of the peptide. Amino acids at the other face of the peptide are available for interaction with the target molecule. Using this scaffold, we demonstrate that recognition molecules can efficiently be designed in silico toward four structurally unrelated proteins, GFP, IL-1β, IL-2, and IL-6. On solid support, 10 different antibody-mimetic recognition molecules were synthesized. They displayed high affinity and no cross-reactivity, as observed by fluorescence microscopy. Stabilized variants were readily obtained by incorporation of azido acids and propargylglycine followed by cyclization via the Cu(I)-catalyzed alkyne–azide cycloaddition reaction. As this new class of antibody mimics can be designed toward essentially any protein, the concept is believed to be useful to a wide range of technologies. Here, their use in protein separation and in the detection of proteins in a sandwich-type assay is demonstrated. American Chemical Society 2019-01-28 2019-02-27 /pmc/articles/PMC6396188/ /pubmed/30834314 http://dx.doi.org/10.1021/acscentsci.8b00614 Text en Copyright © 2019 American Chemical Society This is an open access article published under an ACS AuthorChoice License (http://pubs.acs.org/page/policy/authorchoice_termsofuse.html) , which permits copying and redistribution of the article or any adaptations for non-commercial purposes.
spellingShingle Hu, Hongxia
Kofoed, Christian
Li, Ming
Gonçalves, Juliana Pereira Lopes
Hansen, Jonas
Wolfram, Martin
Hansen, Axel Kornerup
Friis Hansen, Camilla Hartmann
Diness, Frederik
Schoffelen, Sanne
Meldal, Morten
Computational Evolution of Threonine-Rich β-Hairpin Peptides Mimicking Specificity and Affinity of Antibodies
title Computational Evolution of Threonine-Rich β-Hairpin Peptides Mimicking Specificity and Affinity of Antibodies
title_full Computational Evolution of Threonine-Rich β-Hairpin Peptides Mimicking Specificity and Affinity of Antibodies
title_fullStr Computational Evolution of Threonine-Rich β-Hairpin Peptides Mimicking Specificity and Affinity of Antibodies
title_full_unstemmed Computational Evolution of Threonine-Rich β-Hairpin Peptides Mimicking Specificity and Affinity of Antibodies
title_short Computational Evolution of Threonine-Rich β-Hairpin Peptides Mimicking Specificity and Affinity of Antibodies
title_sort computational evolution of threonine-rich β-hairpin peptides mimicking specificity and affinity of antibodies
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6396188/
https://www.ncbi.nlm.nih.gov/pubmed/30834314
http://dx.doi.org/10.1021/acscentsci.8b00614
work_keys_str_mv AT huhongxia computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies
AT kofoedchristian computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies
AT liming computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies
AT goncalvesjulianapereiralopes computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies
AT hansenjonas computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies
AT wolframmartin computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies
AT hansenaxelkornerup computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies
AT friishansencamillahartmann computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies
AT dinessfrederik computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies
AT schoffelensanne computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies
AT meldalmorten computationalevolutionofthreoninerichbhairpinpeptidesmimickingspecificityandaffinityofantibodies

Ejemplares similares