Dynamic Study of Blood–Brain Barrier Closure after its Disruption using Ultrasound: A Quantitative Analysis

Author:

Marty Benjamin1,Larrat Benoit12,Van Landeghem Maxime3,Robic Caroline4,Robert Philippe4,Port Marc4,Le Bihan Denis1,Pernot Mathieu2,Tanter Mickael2,Lethimonnier Franck1,Mériaux Sébastien1

Affiliation:

1. NeuroSpin, I2BM, Commissariat à l’Énergie Atomique, Gif-sur-Yvette, France

2. Institut Langevin, ESPCI ParisTech, CNRS UMR 7587, INSERM U979, Paris, France

3. PPMD, ESPCI ParisTech, CNRS UMR 7615, Paris, France

4. Guerbet Research Division, Roissy-Charles de Gaulle, France

Abstract

Delivery of therapeutic or diagnostic agents to the brain is majorly hindered by the blood–brain barrier (BBB). Recently, many studies have demonstrated local and transient disruption of the BBB using low power ultrasound sonication combined with intravascular microbubbles. However, BBB opening and closure mechanisms are poorly understood, especially the maximum gap that may be safely generated between endothelial cells and the duration of opening of the BBB. Here, we studied BBB opening and closure under magnetic resonance (MR) guidance in a rat model. First, MR contrast agents (CA) of different hydrodynamic diameters (1 to 65 nm) were employed to estimate the largest molecular size permissible across the cerebral tissues. Second, to estimate the duration of the BBB opening, the CA were injected at various times post-BBB disruption (12 minutes to 24 hours). A T1 mapping strategy was developed to assess CA concentration at the ultrasound (US) focal point. Based on our experimental data and BBB closure modeling, a calibration curve was obtained to compute the half closure time as a function of CA hydrodynamic diameter. These findings and the model provide an invaluable basis for optimal design and delivery of nanoparticles to the brain.

Publisher

SAGE Publications

Subject

Cardiology and Cardiovascular Medicine,Neurology (clinical),Neurology

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