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Development of an adenovirus vector vaccine platform for targeting dendritic cells

Adenoviral (Ad) vector vaccines represent one of the most promising modern vaccine platforms, and Ad vector vaccines are currently being investigated in human clinical trials for infectious disease and cancer. Our studies have shown that specific targeting of adenovirus to dendritic cells dramatical...

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Autores principales: Sharma, Piyush K, Dmitriev, Igor P, Kashentseva, Elena A, Raes, Geert, Li, Lijin, Kim, Samuel W, Lu, Zhi-Hong, Arbeit, Jeffrey M, Fleming, Timothy P, Kaliberov, Sergey A, Goedegebuure, S Peter, Curiel, David T, Gillanders, William E
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5972836/
https://www.ncbi.nlm.nih.gov/pubmed/29242639
http://dx.doi.org/10.1038/s41417-017-0002-1
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author Sharma, Piyush K
Dmitriev, Igor P
Kashentseva, Elena A
Raes, Geert
Li, Lijin
Kim, Samuel W
Lu, Zhi-Hong
Arbeit, Jeffrey M
Fleming, Timothy P
Kaliberov, Sergey A
Goedegebuure, S Peter
Curiel, David T
Gillanders, William E
author_facet Sharma, Piyush K
Dmitriev, Igor P
Kashentseva, Elena A
Raes, Geert
Li, Lijin
Kim, Samuel W
Lu, Zhi-Hong
Arbeit, Jeffrey M
Fleming, Timothy P
Kaliberov, Sergey A
Goedegebuure, S Peter
Curiel, David T
Gillanders, William E
author_sort Sharma, Piyush K
collection PubMed
description Adenoviral (Ad) vector vaccines represent one of the most promising modern vaccine platforms, and Ad vector vaccines are currently being investigated in human clinical trials for infectious disease and cancer. Our studies have shown that specific targeting of adenovirus to dendritic cells dramatically enhanced vaccine efficacy. However, this was achieve using a molecular adapter, thereby necessitating a two component vector approach. To address the mandates of clinical translation of our strategy, we here sought to accomplish the goal of DC targeting with a single component adenovirus vector approach. To redirect the specificity of Ad vector vaccines, we replaced the Ad fiber knob with fiber-fibritin chimeras fused to DC1.8, a single domain antibody (sdAb) specific for murine immature DC. We engineered a fiber-fibritin-sdAb chimeric molecule using the coding sequence for DC1.8, and then replaced the native Ad5 fiber knob sequence by homologous recombination. The resulting Ad5 virus, Ad5FF1.8, expresses the chimeric fiber-fibritin sdAb chimera. Infection with Ad5FF1.8 dramatically enhances transgene expression in DC 2.4 dendritic cells compared to infection with native Ad5. Ad5FF1.8 infection of bone marrow derived DC demonstrates that Ad5FF1.8 selectively infects immature DC consistent with the known specificity of DC1.8. Thus, sdAb can be used to selectively redirect the tropism of Ad5 vector vaccines, providing the opportunity to engineer Ad vector vaccines that are specifically targeted to DC, or specific DC subsets.
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spelling pubmed-59728362018-06-15 Development of an adenovirus vector vaccine platform for targeting dendritic cells Sharma, Piyush K Dmitriev, Igor P Kashentseva, Elena A Raes, Geert Li, Lijin Kim, Samuel W Lu, Zhi-Hong Arbeit, Jeffrey M Fleming, Timothy P Kaliberov, Sergey A Goedegebuure, S Peter Curiel, David T Gillanders, William E Cancer Gene Ther Article Adenoviral (Ad) vector vaccines represent one of the most promising modern vaccine platforms, and Ad vector vaccines are currently being investigated in human clinical trials for infectious disease and cancer. Our studies have shown that specific targeting of adenovirus to dendritic cells dramatically enhanced vaccine efficacy. However, this was achieve using a molecular adapter, thereby necessitating a two component vector approach. To address the mandates of clinical translation of our strategy, we here sought to accomplish the goal of DC targeting with a single component adenovirus vector approach. To redirect the specificity of Ad vector vaccines, we replaced the Ad fiber knob with fiber-fibritin chimeras fused to DC1.8, a single domain antibody (sdAb) specific for murine immature DC. We engineered a fiber-fibritin-sdAb chimeric molecule using the coding sequence for DC1.8, and then replaced the native Ad5 fiber knob sequence by homologous recombination. The resulting Ad5 virus, Ad5FF1.8, expresses the chimeric fiber-fibritin sdAb chimera. Infection with Ad5FF1.8 dramatically enhances transgene expression in DC 2.4 dendritic cells compared to infection with native Ad5. Ad5FF1.8 infection of bone marrow derived DC demonstrates that Ad5FF1.8 selectively infects immature DC consistent with the known specificity of DC1.8. Thus, sdAb can be used to selectively redirect the tropism of Ad5 vector vaccines, providing the opportunity to engineer Ad vector vaccines that are specifically targeted to DC, or specific DC subsets. 2017-12-15 2018-02 /pmc/articles/PMC5972836/ /pubmed/29242639 http://dx.doi.org/10.1038/s41417-017-0002-1 Text en Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Sharma, Piyush K
Dmitriev, Igor P
Kashentseva, Elena A
Raes, Geert
Li, Lijin
Kim, Samuel W
Lu, Zhi-Hong
Arbeit, Jeffrey M
Fleming, Timothy P
Kaliberov, Sergey A
Goedegebuure, S Peter
Curiel, David T
Gillanders, William E
Development of an adenovirus vector vaccine platform for targeting dendritic cells
title Development of an adenovirus vector vaccine platform for targeting dendritic cells
title_full Development of an adenovirus vector vaccine platform for targeting dendritic cells
title_fullStr Development of an adenovirus vector vaccine platform for targeting dendritic cells
title_full_unstemmed Development of an adenovirus vector vaccine platform for targeting dendritic cells
title_short Development of an adenovirus vector vaccine platform for targeting dendritic cells
title_sort development of an adenovirus vector vaccine platform for targeting dendritic cells
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5972836/
https://www.ncbi.nlm.nih.gov/pubmed/29242639
http://dx.doi.org/10.1038/s41417-017-0002-1
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