Evaluating baculovirus as a vector for human prostate cancer gene therapy.

Evaluating baculovirus as a vector for human prostate cancer gene therapy.

Gene therapy represents an attractive strategy for the non-invasive treatment of prostate cancer, where current clinical interventions show limited efficacy. Here, we evaluate the use of the insect virus, baculovirus (BV), as a novel vector for human prostate cancer gene therapy. Since prostate tumo...

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Main Authors: Stephanie L Swift, Guillermo C Rivera, Vincent Dussupt, Regina M Leadley, Lucy C Hudson, Corrina Ma de Ridder, Robert Kraaij, Julie E Burns, Norman J Maitland, Lindsay J Georgopoulos
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3675042?pdf=render
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spelling doaj-2b44e3f412824eb893a9ff1215f03de62020-11-24T21:49:44ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0186e6555710.1371/journal.pone.0065557Evaluating baculovirus as a vector for human prostate cancer gene therapy.Stephanie L SwiftGuillermo C RiveraVincent DussuptRegina M LeadleyLucy C HudsonCorrina Ma de RidderRobert KraaijJulie E BurnsNorman J MaitlandLindsay J GeorgopoulosGene therapy represents an attractive strategy for the non-invasive treatment of prostate cancer, where current clinical interventions show limited efficacy. Here, we evaluate the use of the insect virus, baculovirus (BV), as a novel vector for human prostate cancer gene therapy. Since prostate tumours represent a heterogeneous environment, a therapeutic approach that achieves long-term regression must be capable of targeting multiple transformed cell populations. Furthermore, discrimination in the targeting of malignant compared to non-malignant cells would have value in minimising side effects. We employed a number of prostate cancer models to analyse the potential for BV to achieve these goals. In vitro, both traditional prostate cell lines as well as primary epithelial or stromal cells derived from patient prostate biopsies, in two- or three-dimensional cultures, were used. We also evaluated BV in vivo in murine prostate cancer xenograft models. BV was capable of preferentially transducing invasive malignant prostate cancer cell lines compared to early stage cancers and non-malignant samples, a restriction that was not a function of nuclear import. Of more clinical relevance, primary patient-derived prostate cancer cells were also efficiently transduced by BV, with robust rates observed in epithelial cells of basal phenotype, which expressed BV-encoded transgenes faster than epithelial cells of a more differentiated, luminal phenotype. Maximum transduction capacity was observed in stromal cells. BV was able to penetrate through three-dimensional structures, including in vitro spheroids and in vivo orthotopic xenografts. BV vectors containing a nitroreductase transgene in a gene-directed enzyme pro-drug therapy approach were capable of efficiently killing malignant prostate targets following administration of the pro-drug, CB1954. Thus, BV is capable of transducing a large proportion of prostate cell types within a heterogeneous 3-D prostate tumour, can facilitate cell death using a pro-drug approach, and shows promise as a vector for the treatment of prostate cancer.http://europepmc.org/articles/PMC3675042?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Stephanie L Swift
Guillermo C Rivera
Vincent Dussupt
Regina M Leadley
Lucy C Hudson
Corrina Ma de Ridder
Robert Kraaij
Julie E Burns
Norman J Maitland
Lindsay J Georgopoulos
spellingShingle Stephanie L Swift
Guillermo C Rivera
Vincent Dussupt
Regina M Leadley
Lucy C Hudson
Corrina Ma de Ridder
Robert Kraaij
Julie E Burns
Norman J Maitland
Lindsay J Georgopoulos
Evaluating baculovirus as a vector for human prostate cancer gene therapy.
PLoS ONE
author_facet Stephanie L Swift
Guillermo C Rivera
Vincent Dussupt
Regina M Leadley
Lucy C Hudson
Corrina Ma de Ridder
Robert Kraaij
Julie E Burns
Norman J Maitland
Lindsay J Georgopoulos
author_sort Stephanie L Swift
title Evaluating baculovirus as a vector for human prostate cancer gene therapy.
title_short Evaluating baculovirus as a vector for human prostate cancer gene therapy.
title_full Evaluating baculovirus as a vector for human prostate cancer gene therapy.
title_fullStr Evaluating baculovirus as a vector for human prostate cancer gene therapy.
title_full_unstemmed Evaluating baculovirus as a vector for human prostate cancer gene therapy.
title_sort evaluating baculovirus as a vector for human prostate cancer gene therapy.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Gene therapy represents an attractive strategy for the non-invasive treatment of prostate cancer, where current clinical interventions show limited efficacy. Here, we evaluate the use of the insect virus, baculovirus (BV), as a novel vector for human prostate cancer gene therapy. Since prostate tumours represent a heterogeneous environment, a therapeutic approach that achieves long-term regression must be capable of targeting multiple transformed cell populations. Furthermore, discrimination in the targeting of malignant compared to non-malignant cells would have value in minimising side effects. We employed a number of prostate cancer models to analyse the potential for BV to achieve these goals. In vitro, both traditional prostate cell lines as well as primary epithelial or stromal cells derived from patient prostate biopsies, in two- or three-dimensional cultures, were used. We also evaluated BV in vivo in murine prostate cancer xenograft models. BV was capable of preferentially transducing invasive malignant prostate cancer cell lines compared to early stage cancers and non-malignant samples, a restriction that was not a function of nuclear import. Of more clinical relevance, primary patient-derived prostate cancer cells were also efficiently transduced by BV, with robust rates observed in epithelial cells of basal phenotype, which expressed BV-encoded transgenes faster than epithelial cells of a more differentiated, luminal phenotype. Maximum transduction capacity was observed in stromal cells. BV was able to penetrate through three-dimensional structures, including in vitro spheroids and in vivo orthotopic xenografts. BV vectors containing a nitroreductase transgene in a gene-directed enzyme pro-drug therapy approach were capable of efficiently killing malignant prostate targets following administration of the pro-drug, CB1954. Thus, BV is capable of transducing a large proportion of prostate cell types within a heterogeneous 3-D prostate tumour, can facilitate cell death using a pro-drug approach, and shows promise as a vector for the treatment of prostate cancer.
url http://europepmc.org/articles/PMC3675042?pdf=render
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