4.5 Article

Tyrosine-Based Cross-Linking of Peptide Antigens to Generate Nanoclusters with Enhanced Immunogenicity: Demonstration Using the Conserved M2e Peptide of Influenza A

Journal

ACS INFECTIOUS DISEASES
Volume 7, Issue 9, Pages 2723-2735

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsinfecdis.1c00219

Keywords

antigen; influenza; M2e; peptide; tyrosine cross-linking; vaccine

Funding

  1. National Institutes of Health (NIH) [R01AI137846]
  2. Texas Tech University Whitacre Endowed Chair in Science and Engineering

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This study describes a method of creating nanoclusters (NCs) from soluble peptide molecules using a tyrosine-tyrosine cross-linking reaction. The introduction of a reactive tag comprising histidine and tyrosine residues at the termini of the peptide molecules led to the formation of peptide NCs. The study demonstrates the importance of reaction conditions on final cluster diameter and the ability to generate NCs of various sizes. Furthermore, the created peptide clusters show promising immunogenic potential against a lethal influenza A challenge in BALB/c mice.
A method of creating nanoclusters (NCs) from soluble peptide molecules is described utilizing an approach based on a tyrosine-tyrosine cross-linking reaction. A reactive tag comprising histidine and tyrosine residues was introduced at the termini of the peptide molecules. The cross-linking reaction led to the creation of dityrosine bonds within the tag, which allowed for the generation of peptide NCs. We show that it is essential for the reactive tag to be present at both the N and C termini of the peptide for cluster formation to occur. Additionally, the cross-linking reaction was systematically characterized to show the importance of reaction conditions on final cluster diameter, allowing us to generate NCs of various sizes. To demonstrate the immunogenic potential of the peptide clusters, we chose to study the conserved influenza peptide, M2e, as the antigen. M2e NCs were formulated using the cross-linking reaction. We show the ability of the clusters to generate protective immunity in a dose, size, and frequency dependent manner against a lethal influenza A challenge in BALB/c mice. Taken together, the data presented suggest this new cluster formation technique can generate highly immunogenic peptide NCs in a simple and controllable manner.

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