Pitt Shield

Role for caveolin-mediated transcytosis in facilitating transport of large cargoes into the brain via ultrasound.

Authors: Pandit R, Koh WK, Sullivan RKP, Palliyaguru T, Parton RG, Götz J

The blood-brain barrier (BBB) is a dynamic diffusional barrier regulating the molecular and chemical flux between the blood and brain, thereby preserving cerebral homeostasis. Endothelial cells form the core anatomical component of the BBB based on properties such as specialized junctional complexes between cells, which restricts paracellular transport, and extremely low levels of vesicular transport, restricting transcytosis. In performing its protective function, the BBB also constrains the entry of therapeutics into the brain, hampering the treatment of various neurological disorders. Focused ultrasound is a novel therapeutic modality that has shown efficacy in transiently and non-invasively opening the BBB for the targeted delivery of therapeutics to the brain. Although the ability of ultrasound to disrupt the junctional assembly of endothelial cells has been partially investigated, its effect on the transcellular mode of transport has been largely neglected. In this study, we found that ultrasound induces a pronounced increase in the levels of the vesicle-forming protein caveolin-1. In order to investigate the role of vesicle-mediated transcytoplasmic transport, we compared the leakage of various cargo sizes between a mouse model that lacks caveolin-1 and wild-type mice following sonication of the hippocampus. The absence of caveolin-1 did not lead to overt abnormalities in the cerebral vasculature in the mice. We found that caveolin-1 has a critical role specifically in the transport of large (500 kDa), but not smaller (3 and 70 kDa) cargoes. Our findings indicate differential effects of therapeutic ultrasound on cellular transport mechanisms, with implications for therapeutic interventions.

Introduction

Purpose Drug delivery with BBB opening
Study Objective To determine whether caveolin-mediated transcytosis facilitates the transport of large cargoes into the brain during ultrasound-mediated blood–brain barrier disruption.
Animal model / Human subject Mice (Cav1-/-, C57BL/6J); 3 months old; male
Disease model Healthy
Targeted brain region(s) Hippocampus
Target coordinates 2 mm above lambdoid suture; 2.5 mm left of sagittal suture; 2 mm beneath skull
Cargo name and characteristics Dextrans (3 kDa, 70 kDa, 500 kDa, 2000 kDa)
Route of administration retro-orbitally

Outcomes and Safety

Summary of Outcomes FUS promoted caveolin-1 in the sonicatied hippocampus and enabled BBB opening; delivery of 500 kDa dextran was reduced in Cav1-/- mice, but 3, 70 kDa dextrans were unaffected.
Safety-related matter Not reported

Brain Region

Ultrasound Parameters

Ultrasound instrument Integrated FUS system with a center freequency of 1.5 MHz (Therapy Imaging Probe System, TIPS, Philips Research)
FUS Frequency 1.5 MHz
FUS Pressure 0.6 MPa
FUS Mode pulsed
Pulse duration 10 ms
Duration of a single FUS session 1 minute
Focal Characteristics Focal depth: 2 mm, Focal length: 80 mm, Aperture size: 31 mm
Treatment frequency Single

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