Combined effects of scanning ultrasound and a tau-specific single chain antibody in a tau transgenic mouse model.

Alzheimer's disease is characterized by the deposition of amyloid-β as extracellular plaques and hyperphosphorylated tau as intracellular neurofibrillary tangles. Tau pathology characterizes not only Alzheimer's disease, but also many other tauopathies, presenting tau as an attractive therapeutic target. Passive tau immunotherapy has been previously explored; however, because only a small fraction of peripherally delivered antibodies crosses the blood-brain barrier, enters the brain and engages with tau that forms intracellular aggregates, more efficient ways of antibody delivery and neuronal uptake are warranted. In the brain, tau exists as multiple isoforms. Here, we investigated the efficacy of a novel 2N tau isoform-specific single chain antibody fragment, RN2N, delivered by passive immunization in the P301L human tau transgenic pR5 mouse model. We demonstrate that, in treated mice, RN2N reduces anxiety-like behaviour and phosphorylation of tau at distinct sites. When administration of RN2N was combined with focused ultrasound in a scanning mode (scanning ultrasound), RN2N delivery into the brain and uptake by neurons were markedly increased, and efficacy was significantly enhanced. Our study provides evidence that scanning ultrasound is a viable tool to enhance the delivery of biologics across the blood-brain barrier and improve therapeutic outcomes and further presents single-chain antibodies as an alternative to full-length antibodies.

Introduction

Purpose Drug delivery with BBB opening

Study Objective To evaluate whether the 2N tau isoform-specific single-chain antibody fragment RN2N, delivered peripherally and with scanning focused ultrasound, can be transported across the blood–brain barrier into neurons and reduce tau pathology and anxiety-like behaviour in a tau transgenic mouse model.

Animal model / Human subject Mouse, P301L human tau transgenic pR5, age 4.5 months, sex female

Disease model Alzheimer's disease / tauopathy (P301L human tau transgenic mouse model)

Targeted brain region(s) Forebrain; Amygdala; Hippocampus; Cortex

Cargo name and characteristics RN2N — 2N tau isoform-specific single-chain antibody fragment (single-chain variable fragment, scFv), protein biologic delivered by passive immunization

Route of administration retro-orbitally

Outcomes and Safety

Summary of Outcomes Passive immunization with a 2N-tau-specific scFv (RN2N) reduced anxiety-like behaviour and decreased tau phosphorylation (notably AT8 and AT180, with partial reduction of 12E8) in pR5 tau transgenic mice; these effects were markedly enhanced when RN2N delivery was combined with focused scanning ultrasound. The successful ultrasound approach was scanning ultrasound (SUS) with microbubbles to open the blood–brain barrier (safe settings), which increased brain RN2N levels (~11-fold) and neuronal uptake, yielding greater reductions in p-tau than RN2N or SUS alone.

Duration of biological effect 4 weeks

Safety-related matter SUS was conducted using settings previously shown to cause no damage and anaesthesia alone did not affect behaviour, with no adverse effects reported in treated mice. The authors additionally note a safety consideration that ultrasound-mediated delivery may have a size limit for cargos.

Brain Region

Ultrasound Parameters

Ultrasound instrument Therapy Imaging Probe System (TIPS, Philips Research), which has an eight element annular array transducer

FUS Frequency 1 MHz

FUS Pressure 0.7 MPa

FUS Mode pulsed

Pulse duration 10 ms

Duration of a single FUS session 6 s per spot

Focal Characteristics Focal depth: 80 mm; Focal length: 80 mm; Aperture size: 33 mm

Treatment frequency multiple sessions

We are open to feedback. If you see a mistake or have a suggestion, please contact us.