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Capsid Serotype and Timing of Injection Determines AAV Transduction in the Neonatal Mice Brain

Adeno-associated virus (AAV) mediated gene expression is a powerful tool for gene therapy and preclinical studies. A comprehensive analysis of CNS cell type tropism, expression levels and biodistribution of different capsid serotypes has not yet been undertaken in neonatal rodents. Our previous stud...

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Autores principales: Chakrabarty, Paramita, Rosario, Awilda, Cruz, Pedro, Siemienski, Zoe, Ceballos-Diaz, Carolina, Crosby, Keith, Jansen, Karen, Borchelt, David R., Kim, Ji-Yoen, Jankowsky, Joanna L., Golde, Todd E., Levites, Yona
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3692458/
https://www.ncbi.nlm.nih.gov/pubmed/23825679
http://dx.doi.org/10.1371/journal.pone.0067680
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author Chakrabarty, Paramita
Rosario, Awilda
Cruz, Pedro
Siemienski, Zoe
Ceballos-Diaz, Carolina
Crosby, Keith
Jansen, Karen
Borchelt, David R.
Kim, Ji-Yoen
Jankowsky, Joanna L.
Golde, Todd E.
Levites, Yona
author_facet Chakrabarty, Paramita
Rosario, Awilda
Cruz, Pedro
Siemienski, Zoe
Ceballos-Diaz, Carolina
Crosby, Keith
Jansen, Karen
Borchelt, David R.
Kim, Ji-Yoen
Jankowsky, Joanna L.
Golde, Todd E.
Levites, Yona
author_sort Chakrabarty, Paramita
collection PubMed
description Adeno-associated virus (AAV) mediated gene expression is a powerful tool for gene therapy and preclinical studies. A comprehensive analysis of CNS cell type tropism, expression levels and biodistribution of different capsid serotypes has not yet been undertaken in neonatal rodents. Our previous studies show that intracerebroventricular injection with AAV2/1 on neonatal day P0 results in widespread CNS expression but the biodistribution is limited if injected beyond neonatal day P1. To extend these observations we explored the effect of timing of injection on tropism and biodistribution of six commonly used pseudotyped AAVs delivered in the cerebral ventricles of neonatal mice. We demonstrate that AAV2/8 and 2/9 resulted in the most widespread biodistribution in the brain. Most serotypes showed varying biodistribution depending on the day of injection. Injection on neonatal day P0 resulted in mostly neuronal transduction, whereas administration in later periods of development (24–84 hours postnatal) resulted in more non-neuronal transduction. AAV2/5 showed widespread transduction of astrocytes irrespective of the time of injection. None of the serotypes tested showed any microglial transduction. This study demonstrates that both capsid serotype and timing of injection influence the regional and cell-type distribution of AAV in neonatal rodents, and emphasizes the utility of pseudotyped AAV vectors for translational gene therapy paradigms.
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spelling pubmed-36924582013-07-02 Capsid Serotype and Timing of Injection Determines AAV Transduction in the Neonatal Mice Brain Chakrabarty, Paramita Rosario, Awilda Cruz, Pedro Siemienski, Zoe Ceballos-Diaz, Carolina Crosby, Keith Jansen, Karen Borchelt, David R. Kim, Ji-Yoen Jankowsky, Joanna L. Golde, Todd E. Levites, Yona PLoS One Research Article Adeno-associated virus (AAV) mediated gene expression is a powerful tool for gene therapy and preclinical studies. A comprehensive analysis of CNS cell type tropism, expression levels and biodistribution of different capsid serotypes has not yet been undertaken in neonatal rodents. Our previous studies show that intracerebroventricular injection with AAV2/1 on neonatal day P0 results in widespread CNS expression but the biodistribution is limited if injected beyond neonatal day P1. To extend these observations we explored the effect of timing of injection on tropism and biodistribution of six commonly used pseudotyped AAVs delivered in the cerebral ventricles of neonatal mice. We demonstrate that AAV2/8 and 2/9 resulted in the most widespread biodistribution in the brain. Most serotypes showed varying biodistribution depending on the day of injection. Injection on neonatal day P0 resulted in mostly neuronal transduction, whereas administration in later periods of development (24–84 hours postnatal) resulted in more non-neuronal transduction. AAV2/5 showed widespread transduction of astrocytes irrespective of the time of injection. None of the serotypes tested showed any microglial transduction. This study demonstrates that both capsid serotype and timing of injection influence the regional and cell-type distribution of AAV in neonatal rodents, and emphasizes the utility of pseudotyped AAV vectors for translational gene therapy paradigms. Public Library of Science 2013-06-25 /pmc/articles/PMC3692458/ /pubmed/23825679 http://dx.doi.org/10.1371/journal.pone.0067680 Text en © 2013 Chakrabarty 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
Chakrabarty, Paramita
Rosario, Awilda
Cruz, Pedro
Siemienski, Zoe
Ceballos-Diaz, Carolina
Crosby, Keith
Jansen, Karen
Borchelt, David R.
Kim, Ji-Yoen
Jankowsky, Joanna L.
Golde, Todd E.
Levites, Yona
Capsid Serotype and Timing of Injection Determines AAV Transduction in the Neonatal Mice Brain
title Capsid Serotype and Timing of Injection Determines AAV Transduction in the Neonatal Mice Brain
title_full Capsid Serotype and Timing of Injection Determines AAV Transduction in the Neonatal Mice Brain
title_fullStr Capsid Serotype and Timing of Injection Determines AAV Transduction in the Neonatal Mice Brain
title_full_unstemmed Capsid Serotype and Timing of Injection Determines AAV Transduction in the Neonatal Mice Brain
title_short Capsid Serotype and Timing of Injection Determines AAV Transduction in the Neonatal Mice Brain
title_sort capsid serotype and timing of injection determines aav transduction in the neonatal mice brain
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3692458/
https://www.ncbi.nlm.nih.gov/pubmed/23825679
http://dx.doi.org/10.1371/journal.pone.0067680
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