Ultrasound-mediated blood-brain/blood-tumor barrier disruption improves outcomes with trastuzumab in a breast cancer brain metastasis model.
Authors: Park EJ, Zhang YZ, Vykhodtseva N, McDannold N
Trastuzumab has shown positive results in many patients with metastatic HER2-positive breast cancer, but it is less effective for controlling metastases in the CNS, which remains a site of relapse. The poor prognosis for patients with brain metastases is thought to be largely due to the presence of the blood-brain barrier (BBB) that prevents delivery of most drugs to the CNS and to the heterogeneous and limited permeability of the blood-tumor barrier (BTB). Focused ultrasound (FUS) bursts combined with circulating microbubbles can temporarily permeabilize both the BBB and the BTB. This technique has been investigated as a potential noninvasive method for targeted drug delivery in the brain. Here, we investigated whether BBB/BTB permeabilization in the tumor and surrounding brain tissue induced by FUS and microbubbles can slow tumor growth and improve survival in a breast cancer brain metastases model. HER2/neu-positive human breast cancer cells (BT474) were inoculated in the brains of 41 nude (nu/nu) rats. Animals in the treatment group received six weekly treatments of BTB/BBB permeabilization under MRI guidance combined with IV administration of trastuzumab (2 mg/kg). Tumor growth and survival rates were monitored via MRI for seven weeks after sonication. Starting at week seven and continuing through the end of the study, the mean tumor volume of the FUS+trastuzumab group was significantly (P<0.05) less than those of the three control groups (no treatment, FUS alone, trastuzumab alone). Furthermore, in four out of 10 rats treated with FUS+trastuzumab, the tumor appeared to be completely resolved in MRI, an outcome which was not observed in any of the 31 rats in three control groups. Trastuzumab improved median survival by 13% compared to the no treatment group, a difference which was significant (P=0.044). Treatment with FUS+trastuzumab produced the most significant benefit compared to the no-treatment controls (P=0.0084). More than half (6/10) animals survived at the study endpoint, leading to a median survival time greater than 83 days (at least 32% longer than the untreated control group). Overall, this work suggests that BBB/BTB permeabilization induced by FUS and microbubbles can improve outcomes in breast cancer brain metastases.
Introduction
Purpose
Drug delivery with BBB opening
Study Objective
To determine whether focused ultrasound- and microbubble-induced BBB/BTB permeabilization combined with intravenous trastuzumab can slow tumor growth and improve survival in a HER2-positive breast cancer brain metastasis rat model.
Animal model / Human subject
Rat, nude (nu/nu); age 6 weeks old; sex male
Disease model
Breast cancer brain metastases (HER2-positive)
MRI or image guidance method
MRI guidance
Targeted brain region(s)
Tumor; Surrounding Brain Tissue Rim
Cargo name and characteristics
Trastuzumab — humanized monoclonal antibody (protein) targeting HER2/neu, administered intravenously (2 mg/kg)
Route of administration
intravenous
Outcomes and Safety
Summary of Outcomes
MRI-guided FUS with microbubbles and trastuzumab as cargo significantly reduced tumor growth, induced complete responses in some animals, and extended survival compared to single-modality treatments.
Duration of biological effect
greater than 83 days
Safety-related matter
The provided text does not report or discuss any safety data or adverse effects related to FUS, microbubbles, or trastuzumab; no adverse events are mentioned.
Brain Region
Ultrasound Parameters
Ultrasound instrument
Air-backed, single-element, spherically-focused transducer
FUS Frequency
690 kHz
FUS Pressure
0.69 Mpa
FUS Mode
pulsed
Pulse duration
10 ms
Focal Characteristics
Focal depth: None; Focal length: None; Aperture size: None
Treatment frequency
multiple
Mechanical index
0.8306623862918074
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