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MR-guided focused ultrasound increases antibody delivery to nonenhancing high-grade glioma.

Authors: Brighi C, Reid L, White AL, Genovesi LA, Kojic M, Millar A, Bruce Z, Day BW, Rose S, Whittaker AK, Puttick S

High-grade glioma (HGG) remains a recalcitrant clinical problem despite many decades of research. A major challenge in improving prognosis is the inability of current therapeutic strategies to address a clinically significant burden of infiltrating tumor cells that extend beyond the margins of the primary tumor mass. Such cells cannot be surgically excised nor efficiently targeted by radiation therapy. Therapeutic targeting of this tumor cell population is significantly hampered by the presence of an intact blood-brain barrier (BBB). In this study, we performed a preclinical investigation of the efficiency of MR-guided Focused Ultrasound (FUS) to temporarily disrupt the BBB to allow selective delivery of a tumor-targeting antibody to infiltrating tumor. Structural MRI, dynamic-contrast enhancement MRI, and histology were used to fully characterize the MR-enhancing properties of a patient-derived xenograft (PDX) orthotopic mouse model of HGG and to develop a reproducible, robust model of nonenhancing HGG. PET-CT imaging techniques were then used to evaluate the efficacy of FUS to increase <sup>89</sup>Zr-radiolabeled antibody concentration in nonenhancing HGG regions and adjacent non-targeted tumor tissue. The PDX mouse model of HGG has a significant tumor burden lying behind an intact BBB. Increased antibody uptake in nonenhancing tumor regions is directly proportional to the FUS-targeted volume. FUS locally increased antibody uptake in FUS-targeted regions of the tumor with an intact BBB, while leaving untargeted regions unaffected. FUS exposure successfully allowed temporary BBB disruption, localized to specifically targeted, nonenhancing, infiltrating tumor regions and delivery of a systemically administered antibody was significantly increased.

Introduction

Purpose Drug delivery with BBB opening
Study Objective To evaluate whether MR-guided focused ultrasound can transiently disrupt the blood–brain barrier to enhance delivery of a tumor-targeting antibody to nonenhancing, infiltrating high-grade glioma in a preclinical mouse model.
Animal model / Human subject Mus musculus (mouse), NOD/SCID strain, 6-week-old, female
Disease model High-grade glioma (HGG) / glioblastoma
MRI or image guidance method MRI-guided: T2-weighted MRI images were acquired and imported into the FUS guidance software; the hemispherical transducer was mounted in a 3-axis positioning system aligned with the MRI coordinate space.
Targeted brain region(s) Striatum
Cargo name and characteristics 89Zr-radiolabeled EphA2-targeting monoclonal antibody (EphA2-4B3), murine IgG2a protein produced by hybridoma and purified; labeled with Zirconium-89 for PET imaging
Route of administration Intravenous (tail vein injection)

Outcomes and Safety

Summary of Outcomes MR-guided focused ultrasound transiently and locally disrupted the BBB in non-contrast-enhancing infiltrative HGG regions, significantly increasing uptake of a systemically administered antibody in a volume-dependent manner (with associated local astrocyte and microglial activation) while not increasing uptake in already contrast-enhancing regions; no different FUS parameter sets were reported.
Duration of biological effect 3 days
Safety-related matter FUS-induced BBB disruption produced a localized sterile inflammatory response: significant astrogliosis and microgliosis were observed in FUS-targeted tumor regions (P = .0394 and P = .0083), although H&E showed no overt tumor tissue or vascular damage at 3 days post-treatment.

Brain Region

Ultrasound Parameters

Ultrasound instrument LP-100 FUS instrument (FUS Instruments); 1.1 MHz hemispherical transducer; transducer aperture/diameter: None
FUS Frequency 1.1 MHz
FUS Pressure 0.85 MPa
FUS Mode pulsed
Pulse duration 10 ms
Duration of a single FUS session 120 s
Focal Characteristics Focal depth: None; Focal length: None; Aperture size: None
Treatment frequency single

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