Development and characterization of a human papillomavirus-based nanoparticle carrier for heterologous vaccine antigens

Wang Y, Bartelsen N, Arnold P, Müller-Schmucker S, Weingärtner C, Beutel J, Eichler J, Temchura V, Damm D, Überla K (2025)

Publication Type: Journal article

Publication year: 2025

Journal

Scientific Reports Nature Publishing Group: Open Access Journals - Option B

Book Volume: 15

Article Number: 32927

Journal Issue: 1

DOI: 10.1038/s41598-025-19009-3

Abstract

The display of a repetitive array of antigens on the surface of nanoparticles has been shown to effectively trigger the activation of cognate B cells and to increase humoral immune responses. Building on extensive knowledge from the development and clinical use of virus-like particle (VLP) vaccines against Human Papilloma Viruses (HPV), we developed an HPV-based nanoparticle carrier presenting Human Immunodeficiency Virus Type 1 (HIV-1) envelope glycoprotein (Env) as a heterologous vaccine antigen on the surface. After purification of the L1 capsid protein of HPV-16 from a bacterial expression system and assembly of L1 proteins into VLPs (L1-VLPs), we conjugated HIV-1 Env trimers with the C-terminus to the surface of the nanoparticles (L1-Env) using copper-free click reactions via Dibenzocyclooctyne (DBCO)-terminated linker molecules. These L1-Env nanoparticles activated Env-specific B cells more efficiently than non-conjugated Env in a B cell receptor-dependent manner. In general, immunization of mice with L1-Env nanoparticles resulted in Env- and L1-specific antibody responses without the need for an adjuvant. L1-Env nanoparticles induced significantly higher Env-specific antibody responses in comparison to a control group that received a mixture of Env trimers and uncoupled L1-VLPs. Concurrently, we observed decreased L1-specific antibody responses in comparison to mice that were immunized with uncoupled L1-VLPs suggesting partial shielding of L1 epitopes by conjugated Env trimers. In summary, HPV-based nanoparticles provide an attractive novel approach for combinatorial vaccines against sexually transmitted pathogens.

Authors with CRIS profile

Yu Wang Lehrstuhl für Klinische und Molekulare Virologie Nils Bartelsen Institute of Clinical and Molecular Virology Philipp Arnold Lehrstuhl für Funktionelle und Klinische Anatomie Sandra Müller-Schmucker Institute of Clinical and Molecular Virology Christoph Weingärtner Institute of Clinical and Molecular Virology Jannis Beutel Lehrstuhl für Pharmazeutische Chemie Jutta Eichler Professur für Pharmazeutische Chemie Vladimir Temchura Institute of Clinical and Molecular Virology Dominik Damm Institute of Clinical and Molecular Virology Klaus Überla Lehrstuhl für Klinische und Molekulare Virologie

Additional Organisation(s)

FAU Forschungszentrum Neue Wirkstoffe (FAU NeW)

How to cite

APA:

Wang, Y., Bartelsen, N., Arnold, P., Müller-Schmucker, S., Weingärtner, C., Beutel, J.,... Überla, K. (2025). Development and characterization of a human papillomavirus-based nanoparticle carrier for heterologous vaccine antigens. Scientific Reports, 15(1). https://doi.org/10.1038/s41598-025-19009-3

MLA:

Wang, Yu, et al. "Development and characterization of a human papillomavirus-based nanoparticle carrier for heterologous vaccine antigens." Scientific Reports 15.1 (2025).

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