Literature DB >> 28941260

Glial fibrillary acidic protein promoter determines transgene expression in satellite glial cells following intraganglionic adeno-associated virus delivery in adult rats.

Hongfei Xiang1,2, Hao Xu1,2, Fan Fan3, Seung-Min Shin1, Quinn H Hogan1,4, Hongwei Yu1,4.   

Abstract

Recombinant adeno-associated viral (AAV)-mediated therapeutic gene transfer to dorsal root ganglia (DRG) is an effective and safe tool for treating chronic pain. However, AAV with various constitutively active promoters leads to transgene expression predominantly to neurons, while glial cells are refractory to AAV transduction in the peripheral nervous system. The present study evaluated whether in vivo satellite glial cell (SGC) transduction in the DRG can be enhanced by the SGC-specific GFAP promoter and by using shH10 and shH19, which are engineered capsid variants with Müller glia-prone transduction. Titer-matched AAV6 (as control), AAVshH10, and AAVshH19, all encoding the EGFP driven by the constitutively active CMV promoter, as well as AAV6-EGFP and AAVshH10-EGFP driven by a GFAP promoter (AAV6-GFAP-EGFP and AAVshH10-GFAP-EGFP), were injected into DRG of adult male rats. Neurotropism of gene expression was determined and compared by immunohistochemistry. Results showed that injection of AAV6- and AAVshH10-GFAP-EGFP induces robust EGFP expression selectively in SGCs, whereas injection of either AAVshH10-CMV-EGFP or AAVshH19-CMV-EGFP into DRG resulted in a similar in vivo transduction profile to AAV6-CMV-EGFP, all showing efficient transduction of sensory neurons without significant transduction of glial cell populations. Coinjection of AAV6-CMV-mCherry and AAV6-GFAP-EGFP induces transgene expression in neurons and SGCs separately. This report, together with our prior studies, demonstrates that the GFAP promoter rather than capsid tropism determines selective gene expression in SGCs following intraganglionic AAV delivery in adult rats. A dual AAV system, one with GFAP promoter and the other with CMV promoter, can efficiently express transgenes selectively in neurons versus SGCs.
© 2017 Wiley Periodicals, Inc.

Entities:  

Keywords:  dorsal root ganglion; gene therapy; pain; recombinant adeno-associated virus; satellite glial cells

Mesh:

Substances:

Year:  2017        PMID: 28941260      PMCID: PMC5766685          DOI: 10.1002/jnr.24183

Source DB:  PubMed          Journal:  J Neurosci Res        ISSN: 0360-4012            Impact factor:   4.164


  48 in total

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3.  Identifying local and descending inputs for primary sensory neurons.

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Review 4.  Glia and pain: is chronic pain a gliopathy?

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Journal:  Pain       Date:  2013-06-20       Impact factor: 6.961

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9.  Glial promoter selectivity following AAV-delivery to the immature brain.

Authors:  Georg von Jonquieres; Nadine Mersmann; Claudia Bettina Klugmann; Anne Editha Harasta; Beat Lutz; Orla Teahan; Gary David Housley; Dominik Fröhlich; Eva-Maria Krämer-Albers; Matthias Klugmann
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Review 4.  AAV Targeting of Glial Cell Types in the Central and Peripheral Nervous System and Relevance to Human Gene Therapy.

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Journal:  Front Mol Neurosci       Date:  2021-01-11       Impact factor: 5.639

5.  Satellite glial cells in sensory ganglia express functional transient receptor potential ankyrin 1 that is sensitized in neuropathic and inflammatory pain.

Authors:  Seung Min Shin; Brandon Itson-Zoske; Yongsong Cai; Chensheng Qiu; Bin Pan; Cheryl L Stucky; Quinn H Hogan; Hongwei Yu
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6.  Transmembrane protein 100 is expressed in neurons and glia of dorsal root ganglia and is reduced after painful nerve injury.

Authors:  Hongwei Yu; Seung Min Shin; Fei Wang; Hao Xu; Hongfei Xiang; Yongsong Cai; Brandon Itson-Zoske; Quinn H Hogan
Journal:  Pain Rep       Date:  2018-12-26

7.  Enhanced T-type calcium channel 3.2 activity in sensory neurons contributes to neuropathic-like pain of monosodium iodoacetate-induced knee osteoarthritis.

Authors:  Seung Min Shin; Yongsong Cai; Brandon Itson-Zoske; Chensheng Qiu; Xu Hao; Hongfei Xiang; Quinn H Hogan; Hongwei Yu
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