Pitt Shield

Ultrasound-Mediated Blood-Brain Barrier Opening Improves Whole Brain Gene Delivery in Mice.

Authors: Felix MS, Borloz E, Metwally K, Dauba A, Larrat B, Matagne V, Ehinger Y, Villard L, Novell A, Mensah S, Roux JC

Gene therapy represents a powerful therapeutic tool to treat diseased tissues and provide a durable and effective correction. The central nervous system (CNS) is the target of many gene therapy protocols, but its high complexity makes it one of the most difficult organs to reach, in part due to the blood-brain barrier that protects it from external threats. Focused ultrasound (FUS) coupled with microbubbles appears as a technological breakthrough to deliver therapeutic agents into the CNS. While most studies focus on a specific targeted area of the brain, the present work proposes to permeabilize the entire brain for gene therapy in several pathologies. Our results show that, after i.v. administration and FUS sonication in a raster scan manner, a self-complementary AAV9-CMV-GFP vector strongly and safely infected the whole brain of mice. An increase in vector DNA (19.8 times), GFP mRNA (16.4 times), and GFP protein levels (17.4 times) was measured in whole brain extracts of FUS-treated GFP injected mice compared to non-FUS GFP injected mice. In addition to this increase in GFP levels, on average, a 7.3-fold increase of infected cells in the cortex, hippocampus, and striatum was observed. No side effects were detected in the brain of treated mice. The combining of FUS and AAV-based gene delivery represents a significant improvement in the treatment of neurological genetic diseases.

Introduction

Purpose Drug delivery with BBB opening
Study Objective To assess whether raster-scan focused ultrasound with microbubbles can safely permeabilize the entire brain to enable widespread AAV9-mediated gene delivery and transduction in mice.
Animal model / Human subject Male and female wild-type C57BL/6J mice, 7 weeks old
Disease model Healthy
MRI or image guidance method Stereotaxic
Targeted brain region(s) Whole Brain
Cargo name and characteristics scAAV9-CMV-GFP vector
Route of administration Intravenous (retro-orbital sinus)

Outcomes and Safety

Summary of Outcomes Whole-brain FUS and microbubbles significantly improved the systemic delivery of scAAV9-CMV-GFP vectors. The treatment resulted in massive increases in vector DNA, GFP mRNA, and GFP protein across the brain without inducing tissue damage.
Duration of biological effect 1 month
Safety-related matter Safety evaluations at 24 hours and 1 month post-treatment revealed no signs of hemorrhage, ischemia, apoptosis, neuroinflammation, white matter damage, or abnormal glial reactivity.

Brain Region

Ultrasound Parameters

Ultrasound instrument Concave spherically shaped piezocomposite transducer (Imasonic)
FUS Frequency 1.5 MHz
FUS Pressure 0.65 MPa (0.57 MPa in situ)
FUS Mode pulsed
Pulse duration 100 ms
Duration of a single FUS session 150 s
Focal Characteristics Focal length: 20 mm; Aperture size: 25 mm; Focal depth: 6 mm
Treatment frequency Single session

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