Systemic AAV6-synapsin-GFP administration results in lower liver biodistribution, compared to AAV1&2 and AAV9, with neuronal expression following ultrasound-mediated brain delivery.
Authors: Weber-Adrian D, Kofoed RH, Silburt J, Noroozian Z, Shah K, Burgess A, Rideout S, Kügler S, Hynynen K, Aubert I
Non-surgical gene delivery to the brain can be achieved following intravenous injection of viral vectors coupled with transcranial MRI-guided focused ultrasound (MRIgFUS) to temporarily and locally permeabilize the blood-brain barrier. Vector and promoter selection can provide neuronal expression in the brain, while limiting biodistribution and expression in peripheral organs. To date, the biodistribution of adeno-associated viruses (AAVs) within peripheral organs had not been quantified following intravenous injection and MRIgFUS delivery to the brain. We evaluated the quantity of viral DNA from the serotypes AAV9, AAV6, and a mosaic AAV1&2, expressing green fluorescent protein (GFP) under the neuron-specific synapsin promoter (syn). AAVs were administered intravenously during MRIgFUS targeting to the striatum and hippocampus in mice. The syn promoter led to undetectable levels of GFP expression in peripheral organs. In the liver, the biodistribution of AAV9 and AAV1&2 was 12.9- and 4.4-fold higher, respectively, compared to AAV6. The percentage of GFP-positive neurons in the FUS-targeted areas of the brain was comparable for AAV6-syn-GFP and AAV1&2-syn-GFP. In summary, MRIgFUS-mediated gene delivery with AAV6-syn-GFP had lower off-target biodistribution in the liver compared to AAV9 and AAV1&2, while providing neuronal GFP expression in the striatum and hippocampus.
Introduction
Purpose
Drug delivery with BBB opening
Study Objective
To quantify and compare the peripheral biodistribution and targeted neuronal expression in the brain of AAV serotypes (AAV9, AAV6, and mosaic AAV1&2) delivering syn-GFP following intravenous administration with MRI-guided focused ultrasound to the striatum and hippocampus.
Animal model / Human subject
Mus musculus (mouse), C57BL/6, 13 weeks old, sex not specified
Disease model
healthy
MRI or image guidance method
MRI-guided focused ultrasound (MRIgFUS): targeting selected on 7T MRI T2-weighted images (two hippocampal and one striatal FUS spots, ~1–2 mm resolution); contrast-enhanced T1-weighted MRI used post-FUS to confirm BBB opening; real-time acoustic-emission monitoring with a PVDF hydrophone (sub‑harmonic detection) used to control sonication.
Targeted brain region(s)
Striatum
Cargo name and characteristics
AAV
Route of administration
intravenous
Outcomes and Safety
Summary of Outcomes
MRI-guided focused ultrasound opened the BBB and enabled systemic AAV delivery to neurons in the striatum and hippocampus.
Duration of biological effect
2 weeks
Safety-related matter
No major adverse effects reported.
Brain Region
Ultrasound Parameters
Ultrasound instrument
focused ultrasound transducer
FUS Frequency
1.68 MHz
FUS Intensity
not reported
FUS Pressure
not reported
FUS Mode
pulsed
Pulse duration
10 ms
Duration of a single FUS session
120 s
Treatment frequency
Single session
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