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Spinal subpial delivery of AAV9 enables widespread gene silencing and blocks motoneuron degeneration in ALS

Authors :
Noe Govea-Perez
Zoltán Tomori
Atsushi Miyanohara
PeiXi Chen
Mariana Bravo-Hernández
Wenlian Zhu
Joseph D. Ciacci
Brian K. Kaspar
Dara Ditsworth
Melissa McAlonis-Downes
Thomas D. Glenn
Oleksandr Platoshyn
Vladimír Proks
Samuel L. Pfaff
Stefan Juhas
Don W. Cleveland
Sandrine Da Cruz
Michael R. Navarro
Jana Juhasova
Eric T. Ahrens
Helena Kupcova Skalnikova
Ivo Vanicky
Hana Studenovská
Takahiro Tadokoro
Martin Marsala
Yoshiomi Kobayashi
Shawn P. Driscoll
Silvia Marsala
Shang Gao
Source :
Nat Med, Nature medicine, vol 26, iss 1
Publication Year :
2019

Abstract

Gene silencing with virally delivered shRNA represents a promising approach for treatment of inherited neurodegenerative disorders. In the present study we develop a subpial technique, which we show in adult animals successfully delivers adeno-associated virus (AAV) throughout the cervical, thoracic and lumbar spinal cord, as well as brain motor centers. One-time injection at cervical and lumbar levels just before disease onset in mice expressing a familial amyotrophic lateral sclerosis (ALS)-causing mutant SOD1 produces long-term suppression of motoneuron disease, including near-complete preservation of spinal α-motoneurons and muscle innervation. Treatment after disease onset potently blocks progression of disease and further α-motoneuron degeneration. A single subpial AAV9 injection in adult pigs or non-human primates using a newly designed device produces homogeneous delivery throughout the cervical spinal cord white and gray matter and brain motor centers. Thus, spinal subpial delivery in adult animals is highly effective for AAV-mediated gene delivery throughout the spinal cord and supraspinal motor centers. Injection of AAV–shRNA below the pial surface of the spinal cord prevents onset or ameliorates progression in a mouse model of ALS, and achieves widespread delivery to the spinal cord and brain motor centers in adult pigs and non-human primates.

Details

Language :
English
Database :
OpenAIRE
Journal :
Nat Med, Nature medicine, vol 26, iss 1
Accession number :
edsair.doi.dedup.....86d6e6d341c49955c92f1d93ffac3ebe