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Dendritic Cell Based PSMA Immunotherapy for Prostate Cancer Using a CD40-Targeted Adenovirus Vector

Human prostate tumor vaccine and gene therapy trials using ex vivo methods to prime dendritic cells (DCs) with prostate specific membrane antigen (PSMA) have been somewhat successful, but to date the lengthy ex vivo manipulation of DCs has limited the widespread clinical utility of this approach. Ou...

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Autores principales: Williams, Briana Jill, Bhatia, Shilpa, Adams, Lisa K., Boling, Susan, Carroll, Jennifer L., Li, Xiao-Lin, Rogers, Donna L., Korokhov, Nikolay, Kovesdi, Imre, Pereboev, Alexander V., Curiel, David T., Mathis, J. Michael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3466199/
https://www.ncbi.nlm.nih.gov/pubmed/23056548
http://dx.doi.org/10.1371/journal.pone.0046981
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author Williams, Briana Jill
Bhatia, Shilpa
Adams, Lisa K.
Boling, Susan
Carroll, Jennifer L.
Li, Xiao-Lin
Rogers, Donna L.
Korokhov, Nikolay
Kovesdi, Imre
Pereboev, Alexander V.
Curiel, David T.
Mathis, J. Michael
author_facet Williams, Briana Jill
Bhatia, Shilpa
Adams, Lisa K.
Boling, Susan
Carroll, Jennifer L.
Li, Xiao-Lin
Rogers, Donna L.
Korokhov, Nikolay
Kovesdi, Imre
Pereboev, Alexander V.
Curiel, David T.
Mathis, J. Michael
author_sort Williams, Briana Jill
collection PubMed
description Human prostate tumor vaccine and gene therapy trials using ex vivo methods to prime dendritic cells (DCs) with prostate specific membrane antigen (PSMA) have been somewhat successful, but to date the lengthy ex vivo manipulation of DCs has limited the widespread clinical utility of this approach. Our goal was to improve upon cancer vaccination with tumor antigens by delivering PSMA via a CD40-targeted adenovirus vector directly to DCs as an efficient means for activation and antigen presentation to T-cells. To test this approach, we developed a mouse model of prostate cancer by generating clonal derivatives of the mouse RM-1 prostate cancer cell line expressing human PSMA (RM-1-PSMA cells). To maximize antigen presentation in target cells, both MHC class I and TAP protein expression was induced in RM-1 cells by transduction with an Ad vector expressing interferon-gamma (Ad5-IFNγ). Administering DCs infected ex vivo with CD40-targeted Ad5-huPSMA, as well as direct intraperitoneal injection of the vector, resulted in high levels of tumor-specific CTL responses against RM-1-PSMA cells pretreated with Ad5-IFNγ as target cells. CD40 targeting significantly improved the therapeutic antitumor efficacy of Ad5-huPSMA encoding PSMA when combined with Ad5-IFNγ in the RM-1-PSMA model. These results suggest that a CD-targeted adenovirus delivering PSMA may be effective clinically for prostate cancer immunotherapy.
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spelling pubmed-34661992012-10-10 Dendritic Cell Based PSMA Immunotherapy for Prostate Cancer Using a CD40-Targeted Adenovirus Vector Williams, Briana Jill Bhatia, Shilpa Adams, Lisa K. Boling, Susan Carroll, Jennifer L. Li, Xiao-Lin Rogers, Donna L. Korokhov, Nikolay Kovesdi, Imre Pereboev, Alexander V. Curiel, David T. Mathis, J. Michael PLoS One Research Article Human prostate tumor vaccine and gene therapy trials using ex vivo methods to prime dendritic cells (DCs) with prostate specific membrane antigen (PSMA) have been somewhat successful, but to date the lengthy ex vivo manipulation of DCs has limited the widespread clinical utility of this approach. Our goal was to improve upon cancer vaccination with tumor antigens by delivering PSMA via a CD40-targeted adenovirus vector directly to DCs as an efficient means for activation and antigen presentation to T-cells. To test this approach, we developed a mouse model of prostate cancer by generating clonal derivatives of the mouse RM-1 prostate cancer cell line expressing human PSMA (RM-1-PSMA cells). To maximize antigen presentation in target cells, both MHC class I and TAP protein expression was induced in RM-1 cells by transduction with an Ad vector expressing interferon-gamma (Ad5-IFNγ). Administering DCs infected ex vivo with CD40-targeted Ad5-huPSMA, as well as direct intraperitoneal injection of the vector, resulted in high levels of tumor-specific CTL responses against RM-1-PSMA cells pretreated with Ad5-IFNγ as target cells. CD40 targeting significantly improved the therapeutic antitumor efficacy of Ad5-huPSMA encoding PSMA when combined with Ad5-IFNγ in the RM-1-PSMA model. These results suggest that a CD-targeted adenovirus delivering PSMA may be effective clinically for prostate cancer immunotherapy. Public Library of Science 2012-10-08 /pmc/articles/PMC3466199/ /pubmed/23056548 http://dx.doi.org/10.1371/journal.pone.0046981 Text en © 2012 Williams et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Williams, Briana Jill
Bhatia, Shilpa
Adams, Lisa K.
Boling, Susan
Carroll, Jennifer L.
Li, Xiao-Lin
Rogers, Donna L.
Korokhov, Nikolay
Kovesdi, Imre
Pereboev, Alexander V.
Curiel, David T.
Mathis, J. Michael
Dendritic Cell Based PSMA Immunotherapy for Prostate Cancer Using a CD40-Targeted Adenovirus Vector
title Dendritic Cell Based PSMA Immunotherapy for Prostate Cancer Using a CD40-Targeted Adenovirus Vector
title_full Dendritic Cell Based PSMA Immunotherapy for Prostate Cancer Using a CD40-Targeted Adenovirus Vector
title_fullStr Dendritic Cell Based PSMA Immunotherapy for Prostate Cancer Using a CD40-Targeted Adenovirus Vector
title_full_unstemmed Dendritic Cell Based PSMA Immunotherapy for Prostate Cancer Using a CD40-Targeted Adenovirus Vector
title_short Dendritic Cell Based PSMA Immunotherapy for Prostate Cancer Using a CD40-Targeted Adenovirus Vector
title_sort dendritic cell based psma immunotherapy for prostate cancer using a cd40-targeted adenovirus vector
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3466199/
https://www.ncbi.nlm.nih.gov/pubmed/23056548
http://dx.doi.org/10.1371/journal.pone.0046981
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