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research article

Phage Display Selection against a Mixture of Protein Targets

Kong, Xu‐Dong  
•
Zhang, Meng-Jie
•
Heinis, Christian  
May 26, 2025
ACS Chemical Biology

Affinity selections by phage display or other display techniques are typically performed against single targets immobilized as a purified protein. In order to develop cross-specific binders that engage with multiple proteins, such as members of a related family, we herein propose to perform selections against mixtures of proteins as bait. Combined with follow-up selection rounds against the individual proteins, deep sequencing, and single clone enrichment analysis, we expected to distinguish binders that are cross-specific from those that are not. Indeed, applying the strategy to human and mouse coagulation factor XI (hFXI and mFXI), and thus to a situation with limited complexity due to a mixture of only two targets, allowed rapid identification of peptide-based binders along with precise information about their specificity. The study also provided insights into the dynamics and challenges of multitarget affinity selections, showing that one target can easily dominate the selection process and hinder the enrichment of binders to other proteins in a mixture.

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Type
research article
DOI
10.1021/acschembio.5c00121
Author(s)
Kong, Xu‐Dong  

École Polytechnique Fédérale de Lausanne

Zhang, Meng-Jie

Shanghai Jiao Tong University

Heinis, Christian  

École Polytechnique Fédérale de Lausanne

Date Issued

2025-05-26

Publisher

American Chemical Society (ACS)

Published in
ACS Chemical Biology
Subjects

Chemical specificity

•

Genetics

•

Mixtures

•

Peptides and proteins

•

Viruses

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LPPT  
FunderFunding(s)Grant NumberGrant URL

Swiss National Science Foundation

Development and application of two general methods for creating orally applicable cyclic peptide therapeutics

192368

https://data.snf.ch/grants/grant/192368

H2020 European Research Council

101020521

101020521-TARGET

Available on Infoscience
May 27, 2025
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/250822
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