A tractable covalent linker strategy for the production of immunogenic antigen-TLR7/8L bioconjugates

C. J. Massena; S. K. Lathrop; C. J. Davison; R. Schoener; H. G. Bazin; J. T. Evans; D. J. Burkhart

doi:10.1039/d1cc00795e

A tractable covalent linker strategy for the production of immunogenic antigen-TLR7/8L bioconjugates

C. J. Massena
, S. K. Lathrop
, C. J. Davison
, R. Schoener
, H. G. Bazin
, J. T. Evans
, D. J. Burkhart

Center for Translational Medicine

University of Montana

Research output: Contribution to journal › Article › peer-review

8 Scopus citations

Abstract

Despite the ease of production and improved safety profiles of recombinant vaccines, the inherently low immunogenicity of unadjuvanted proteins remains an impediment to their widespread adoption. The covalent tethering of TLR agonists to antigenic proteins offers a unique approach to co-deliver both constituents to the same cell - enhancing vaccine efficacy while minimizing reactogenicity. However, the paucity of simple and effective linker chemistries continues to hamper progress. Here, we present a modular, PEG-based linker system compatible with even extremely lipophilic and challenging TLR7/8 agonists. To advance the field and address previous obstacles, we offer the most straightforward and antigen-preserving linker system to date. These antigen-adjuvant conjugates enhance antigen-specific immune responses in mice, demonstrating the power of our approach within the context of modern vaccinology.

Original language	English
Pages (from-to)	4698-4701
Number of pages	4
Journal	Chemical Communications
Volume	57
Issue number	38
DOIs	https://doi.org/10.1039/d1cc00795e
State	Published - May 11 2021

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abstract = "Despite the ease of production and improved safety profiles of recombinant vaccines, the inherently low immunogenicity of unadjuvanted proteins remains an impediment to their widespread adoption. The covalent tethering of TLR agonists to antigenic proteins offers a unique approach to co-deliver both constituents to the same cell - enhancing vaccine efficacy while minimizing reactogenicity. However, the paucity of simple and effective linker chemistries continues to hamper progress. Here, we present a modular, PEG-based linker system compatible with even extremely lipophilic and challenging TLR7/8 agonists. To advance the field and address previous obstacles, we offer the most straightforward and antigen-preserving linker system to date. These antigen-adjuvant conjugates enhance antigen-specific immune responses in mice, demonstrating the power of our approach within the context of modern vaccinology.",

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AU - Massena, C. J.

AU - Lathrop, S. K.

AU - Davison, C. J.

AU - Schoener, R.

AU - Bazin, H. G.

AU - Evans, J. T.

AU - Burkhart, D. J.

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AB - Despite the ease of production and improved safety profiles of recombinant vaccines, the inherently low immunogenicity of unadjuvanted proteins remains an impediment to their widespread adoption. The covalent tethering of TLR agonists to antigenic proteins offers a unique approach to co-deliver both constituents to the same cell - enhancing vaccine efficacy while minimizing reactogenicity. However, the paucity of simple and effective linker chemistries continues to hamper progress. Here, we present a modular, PEG-based linker system compatible with even extremely lipophilic and challenging TLR7/8 agonists. To advance the field and address previous obstacles, we offer the most straightforward and antigen-preserving linker system to date. These antigen-adjuvant conjugates enhance antigen-specific immune responses in mice, demonstrating the power of our approach within the context of modern vaccinology.

UR - https://www.scopus.com/pages/publications/85105750392

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ER -

A tractable covalent linker strategy for the production of immunogenic antigen-TLR7/8L bioconjugates

Abstract

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