Switching on the lights for gene therapy.
Strategies for non-invasive and quantitative imaging of gene expression in vivo have been developed over the past decade. Non-invasive assessment of the dynamics of gene regulation is of interest for the detection of endogenous disease-specific biological alterations (e.g., signal transduction) and...
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doaj-bdc0634e2f6943149f9130268f1ef8632020-11-25T01:57:35ZengPublic Library of Science (PLoS)PLoS ONE1932-62032007-01-0126e52810.1371/journal.pone.0000528Switching on the lights for gene therapy.Alexandra WinkelerMiguel Sena-EstevesLeonie E M PaulisHongfeng LiYannic WaerzeggersBenedikt RückriemUwe HimmelreichMarkus KleinParisa MonfaredMaria A RuegerMichael HenekaStefan VollmarMathias HoehnCornel FraefelRudolf GrafKlaus WienhardWolf D HeissAndreas H JacobsStrategies for non-invasive and quantitative imaging of gene expression in vivo have been developed over the past decade. Non-invasive assessment of the dynamics of gene regulation is of interest for the detection of endogenous disease-specific biological alterations (e.g., signal transduction) and for monitoring the induction and regulation of therapeutic genes (e.g., gene therapy). To demonstrate that non-invasive imaging of regulated expression of any type of gene after in vivo transduction by versatile vectors is feasible, we generated regulatable herpes simplex virus type 1 (HSV-1) amplicon vectors carrying hormone (mifepristone) or antibiotic (tetracycline) regulated promoters driving the proportional co-expression of two marker genes. Regulated gene expression was monitored by fluorescence microscopy in culture and by positron emission tomography (PET) or bioluminescence (BLI) in vivo. The induction levels evaluated in glioma models varied depending on the dose of inductor. With fluorescence microscopy and BLI being the tools for assessing gene expression in culture and animal models, and with PET being the technology for possible application in humans, the generated vectors may serve to non-invasively monitor the dynamics of any gene of interest which is proportionally co-expressed with the respective imaging marker gene in research applications aiming towards translation into clinical application.http://europepmc.org/articles/PMC1885827?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Alexandra Winkeler Miguel Sena-Esteves Leonie E M Paulis Hongfeng Li Yannic Waerzeggers Benedikt Rückriem Uwe Himmelreich Markus Klein Parisa Monfared Maria A Rueger Michael Heneka Stefan Vollmar Mathias Hoehn Cornel Fraefel Rudolf Graf Klaus Wienhard Wolf D Heiss Andreas H Jacobs |
spellingShingle |
Alexandra Winkeler Miguel Sena-Esteves Leonie E M Paulis Hongfeng Li Yannic Waerzeggers Benedikt Rückriem Uwe Himmelreich Markus Klein Parisa Monfared Maria A Rueger Michael Heneka Stefan Vollmar Mathias Hoehn Cornel Fraefel Rudolf Graf Klaus Wienhard Wolf D Heiss Andreas H Jacobs Switching on the lights for gene therapy. PLoS ONE |
author_facet |
Alexandra Winkeler Miguel Sena-Esteves Leonie E M Paulis Hongfeng Li Yannic Waerzeggers Benedikt Rückriem Uwe Himmelreich Markus Klein Parisa Monfared Maria A Rueger Michael Heneka Stefan Vollmar Mathias Hoehn Cornel Fraefel Rudolf Graf Klaus Wienhard Wolf D Heiss Andreas H Jacobs |
author_sort |
Alexandra Winkeler |
title |
Switching on the lights for gene therapy. |
title_short |
Switching on the lights for gene therapy. |
title_full |
Switching on the lights for gene therapy. |
title_fullStr |
Switching on the lights for gene therapy. |
title_full_unstemmed |
Switching on the lights for gene therapy. |
title_sort |
switching on the lights for gene therapy. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2007-01-01 |
description |
Strategies for non-invasive and quantitative imaging of gene expression in vivo have been developed over the past decade. Non-invasive assessment of the dynamics of gene regulation is of interest for the detection of endogenous disease-specific biological alterations (e.g., signal transduction) and for monitoring the induction and regulation of therapeutic genes (e.g., gene therapy). To demonstrate that non-invasive imaging of regulated expression of any type of gene after in vivo transduction by versatile vectors is feasible, we generated regulatable herpes simplex virus type 1 (HSV-1) amplicon vectors carrying hormone (mifepristone) or antibiotic (tetracycline) regulated promoters driving the proportional co-expression of two marker genes. Regulated gene expression was monitored by fluorescence microscopy in culture and by positron emission tomography (PET) or bioluminescence (BLI) in vivo. The induction levels evaluated in glioma models varied depending on the dose of inductor. With fluorescence microscopy and BLI being the tools for assessing gene expression in culture and animal models, and with PET being the technology for possible application in humans, the generated vectors may serve to non-invasively monitor the dynamics of any gene of interest which is proportionally co-expressed with the respective imaging marker gene in research applications aiming towards translation into clinical application. |
url |
http://europepmc.org/articles/PMC1885827?pdf=render |
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