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Image-guided focused ultrasound-mediated molecular delivery to breast cancer in an animal model
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作者:

Margolis, Ryan
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h-index: 0
机构:
Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA

Basavarajappa, Lokesh
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Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA

Li, Junjie
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Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA

Obaid, Girgis
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Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA

Hoyt, Kenneth
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Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA
机构:
[1] Univ Texas Dallas, Dept Bioengn, Richardson, TX 75080 USA
关键词:
cancer;
drug delivery;
focused ultrasound;
image-guided therapy;
microbubble contrast agents;
optical imaging;
BLOOD-BRAIN-BARRIER;
NEOADJUVANT CHEMOTHERAPY;
COLORECTAL-CANCER;
THERAPY;
MICROBUBBLES;
DISRUPTION;
RESECTION;
SIZE;
D O I:
10.1088/1361-6560/ace23d
中图分类号:
R318 [生物医学工程];
学科分类号:
0831 ;
摘要:
Tumors become inoperable due to their size or location, making neoadjuvant chemotherapy the primary treatment. However, target tissue accumulation of anticancer agents is limited by the physical barriers of the tumor microenvironment. Low-intensity focused ultrasound (FUS) in combination with microbubble (MB) contrast agents can increase microvascular permeability and improve drug delivery to the target tissue after systemic administration. The goal of this research was to investigate image-guided FUS-mediated molecular delivery in volume space. Three-dimensional (3-D) FUS therapy functionality was implemented on a programmable ultrasound scanner (Vantage 256, Verasonics Inc.) equipped with a linear array for image guidance and a 128-element therapy transducer (HIFUPlex-06, Sonic Concepts). FUS treatment was performed on breast cancer-bearing female mice (N = 25). Animals were randomly divided into three groups, namely, 3-D FUS therapy, two-dimensional (2-D) FUS therapy, or sham (control) therapy. Immediately prior to the application of FUS therapy, animals received a slow bolus injection of MBs (Definity, Lantheus Medical Imaging Inc.) and near-infrared dye (IR-780, surrogate drug) for optical reporting and quantification of molecular delivery. Dye accumulation was monitored via in vivo optical imaging at 0, 1, 24, and 48 h (Pearl Trilogy, LI-COR). Following the 48 h time point, animals were humanely euthanized and tumors excised for ex vivo analyzes. Optical imaging results revealed that 3-D FUS therapy improved delivery of the IR-780 dye by 66.4% and 168.1% at 48 h compared to 2-D FUS (p = 0.18) and sham (p = 0.047) therapeutic strategies, respectively. Ex vivo analysis revealed similar trends. Overall, 3-D FUS therapy can improve accumulation of a surrogate drug throughout the entire target tumor burden after systemic administration.
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