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In Vivo Assembly of Nanoparticles Achieved through Synergy of Structure‐Based Protein Engineering and Synthetic DNA Generates Enhanced Adaptive Immunity

Nanotechnologies are considered to be of growing importance to the vaccine field. Through decoration of immunogens on multivalent nanoparticles, designed nanovaccines can elicit improved humoral immunity. However, significant practical and monetary challenges in large‐scale production of nanovaccine...

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Autores principales: Xu, Ziyang, Wise, Megan C., Chokkalingam, Neethu, Walker, Susanne, Tello‐Ruiz, Edgar, Elliott, Sarah T. C., Perales‐Puchalt, Alfredo, Xiao, Peng, Zhu, Xizhou, Pumroy, Ruth A., Fisher, Paul D., Schultheis, Katherine, Schade, Eric, Menis, Sergey, Guzman, Stacy, Andersen, Hanne, Broderick, Kate E., Humeau, Laurent M., Muthumani, Kar, Moiseenkova‐Bell, Vera, Schief, William R., Weiner, David B., Kulp, Daniel W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7175333/
https://www.ncbi.nlm.nih.gov/pubmed/32328416
http://dx.doi.org/10.1002/advs.201902802
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author Xu, Ziyang
Wise, Megan C.
Chokkalingam, Neethu
Walker, Susanne
Tello‐Ruiz, Edgar
Elliott, Sarah T. C.
Perales‐Puchalt, Alfredo
Xiao, Peng
Zhu, Xizhou
Pumroy, Ruth A.
Fisher, Paul D.
Schultheis, Katherine
Schade, Eric
Menis, Sergey
Guzman, Stacy
Andersen, Hanne
Broderick, Kate E.
Humeau, Laurent M.
Muthumani, Kar
Moiseenkova‐Bell, Vera
Schief, William R.
Weiner, David B.
Kulp, Daniel W.
author_facet Xu, Ziyang
Wise, Megan C.
Chokkalingam, Neethu
Walker, Susanne
Tello‐Ruiz, Edgar
Elliott, Sarah T. C.
Perales‐Puchalt, Alfredo
Xiao, Peng
Zhu, Xizhou
Pumroy, Ruth A.
Fisher, Paul D.
Schultheis, Katherine
Schade, Eric
Menis, Sergey
Guzman, Stacy
Andersen, Hanne
Broderick, Kate E.
Humeau, Laurent M.
Muthumani, Kar
Moiseenkova‐Bell, Vera
Schief, William R.
Weiner, David B.
Kulp, Daniel W.
author_sort Xu, Ziyang
collection PubMed
description Nanotechnologies are considered to be of growing importance to the vaccine field. Through decoration of immunogens on multivalent nanoparticles, designed nanovaccines can elicit improved humoral immunity. However, significant practical and monetary challenges in large‐scale production of nanovaccines have impeded their widespread clinical translation. Here, an alternative approach is illustrated integrating computational protein modeling and adaptive electroporation‐mediated synthetic DNA delivery, thus enabling direct in vivo production of nanovaccines. DNA‐launched nanoparticles are demonstrated displaying an HIV immunogen spontaneously self‐assembled in vivo. DNA‐launched nanovaccines induce stronger humoral responses than their monomeric counterparts in both mice and guinea pigs, and uniquely elicit CD8+ effector T‐cell immunity as compared to recombinant protein nanovaccines. Improvements in vaccine responses recapitulate when DNA‐launched nanovaccines with alternative scaffolds and decorated antigen are designed and evaluated. Finally, evaluation of functional immune responses induced by DLnanovaccines demonstrates that, in comparison to control mice or mice immunized with DNA‐encoded hemagglutinin monomer, mice immunized with a DNA‐launched hemagglutinin nanoparticle vaccine fully survive a lethal influenza challenge, and have substantially lower viral load, weight loss, and influenza‐induced lung pathology. Additional study of these next‐generation in vivo‐produced nanovaccines may offer advantages for immunization against multiple disease targets.
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spelling pubmed-71753332020-04-23 In Vivo Assembly of Nanoparticles Achieved through Synergy of Structure‐Based Protein Engineering and Synthetic DNA Generates Enhanced Adaptive Immunity Xu, Ziyang Wise, Megan C. Chokkalingam, Neethu Walker, Susanne Tello‐Ruiz, Edgar Elliott, Sarah T. C. Perales‐Puchalt, Alfredo Xiao, Peng Zhu, Xizhou Pumroy, Ruth A. Fisher, Paul D. Schultheis, Katherine Schade, Eric Menis, Sergey Guzman, Stacy Andersen, Hanne Broderick, Kate E. Humeau, Laurent M. Muthumani, Kar Moiseenkova‐Bell, Vera Schief, William R. Weiner, David B. Kulp, Daniel W. Adv Sci (Weinh) Full Papers Nanotechnologies are considered to be of growing importance to the vaccine field. Through decoration of immunogens on multivalent nanoparticles, designed nanovaccines can elicit improved humoral immunity. However, significant practical and monetary challenges in large‐scale production of nanovaccines have impeded their widespread clinical translation. Here, an alternative approach is illustrated integrating computational protein modeling and adaptive electroporation‐mediated synthetic DNA delivery, thus enabling direct in vivo production of nanovaccines. DNA‐launched nanoparticles are demonstrated displaying an HIV immunogen spontaneously self‐assembled in vivo. DNA‐launched nanovaccines induce stronger humoral responses than their monomeric counterparts in both mice and guinea pigs, and uniquely elicit CD8+ effector T‐cell immunity as compared to recombinant protein nanovaccines. Improvements in vaccine responses recapitulate when DNA‐launched nanovaccines with alternative scaffolds and decorated antigen are designed and evaluated. Finally, evaluation of functional immune responses induced by DLnanovaccines demonstrates that, in comparison to control mice or mice immunized with DNA‐encoded hemagglutinin monomer, mice immunized with a DNA‐launched hemagglutinin nanoparticle vaccine fully survive a lethal influenza challenge, and have substantially lower viral load, weight loss, and influenza‐induced lung pathology. Additional study of these next‐generation in vivo‐produced nanovaccines may offer advantages for immunization against multiple disease targets. John Wiley and Sons Inc. 2020-02-27 /pmc/articles/PMC7175333/ /pubmed/32328416 http://dx.doi.org/10.1002/advs.201902802 Text en © 2020 The Authors. Published by WILEY‐VCH Verlag GmbH & Co. KGaA, Weinheim This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Full Papers
Xu, Ziyang
Wise, Megan C.
Chokkalingam, Neethu
Walker, Susanne
Tello‐Ruiz, Edgar
Elliott, Sarah T. C.
Perales‐Puchalt, Alfredo
Xiao, Peng
Zhu, Xizhou
Pumroy, Ruth A.
Fisher, Paul D.
Schultheis, Katherine
Schade, Eric
Menis, Sergey
Guzman, Stacy
Andersen, Hanne
Broderick, Kate E.
Humeau, Laurent M.
Muthumani, Kar
Moiseenkova‐Bell, Vera
Schief, William R.
Weiner, David B.
Kulp, Daniel W.
In Vivo Assembly of Nanoparticles Achieved through Synergy of Structure‐Based Protein Engineering and Synthetic DNA Generates Enhanced Adaptive Immunity
title In Vivo Assembly of Nanoparticles Achieved through Synergy of Structure‐Based Protein Engineering and Synthetic DNA Generates Enhanced Adaptive Immunity
title_full In Vivo Assembly of Nanoparticles Achieved through Synergy of Structure‐Based Protein Engineering and Synthetic DNA Generates Enhanced Adaptive Immunity
title_fullStr In Vivo Assembly of Nanoparticles Achieved through Synergy of Structure‐Based Protein Engineering and Synthetic DNA Generates Enhanced Adaptive Immunity
title_full_unstemmed In Vivo Assembly of Nanoparticles Achieved through Synergy of Structure‐Based Protein Engineering and Synthetic DNA Generates Enhanced Adaptive Immunity
title_short In Vivo Assembly of Nanoparticles Achieved through Synergy of Structure‐Based Protein Engineering and Synthetic DNA Generates Enhanced Adaptive Immunity
title_sort in vivo assembly of nanoparticles achieved through synergy of structure‐based protein engineering and synthetic dna generates enhanced adaptive immunity
topic Full Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7175333/
https://www.ncbi.nlm.nih.gov/pubmed/32328416
http://dx.doi.org/10.1002/advs.201902802
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