Noninvasive localized delivery of Herceptin to the mouse brain by MRI-guided focused ultrasound-induced blood–brain barrier disruption

Kinoshita, Manabu; McDannold, Nathan; Jólesz, Ferenc A.; Hynynen, Kullervo

doi:10.1073/pnas.0604318103

Cited by 582 publications

(444 citation statements)

References 29 publications

(45 reference statements)

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“…The first obstacle is the selectively permeable BBB, which hampers the transport and diffusion of large molecules (>500 Da) from the vasculature into the brain, thus reducing the effects of chemotherapeutic agents against the malignant brain tumors 11. Recently, focused ultrasound (FUS) combined with microbubbles (MB), has been increasingly recognized as a noninvasive strategy to induce transient, reversible, and local BBB disruption 12. The biosafety and effectiveness have also been demonstrated by numerous preclinical studies 13.…”

Section: Introductionmentioning

confidence: 99%

Focused Ultrasound‐Augmented Delivery of Biodegradable Multifunctional Nanoplatforms for Imaging‐Guided Brain Tumor Treatment

Chen

et al. 2018

Advanced Science

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The blood brain barrier is the main obstacle to delivering diagnostic and therapeutic agents to the diseased sites of brain. It is still of great challenge for the combined use of focused ultrasound (FUS) and theranostic nanotechnology to achieve noninvasive and localized delivery of chemotherapeutic drugs into orthotopic brain tumor. In this work, a unique theranostic nanoplatform for highly efficient photoacoustic imaging‐guided chemotherapy of brain tumor both in vitro and in vivo, which is based on the utilization of hollow mesoporous organosilica nanoparticles (HMONs) to integrate ultrasmall Cu2− xSe particles on the surface and doxorubicin inside the hollow interior, is synthesized. The developed multifunctional theranostic nanosystems exhibit tumor‐triggered programmed destruction due to the reducing microenvironment‐responsive cleavage of disulfide bonds that are incorporated into the framework of HMONs and linked between HMONs and Cu2− xSe, resulting in tumor‐specific biodegradation and on‐demand drug‐releasing behavior. Such tumor microenvironment‐responsive biodegradable and biocompatible theranostic nanosystems in combination with FUS provide a promising delivery nanoplatform with high performance for orthotopic brain tumor imaging and therapy.

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Section: Introductionmentioning

confidence: 99%

Focused Ultrasound‐Augmented Delivery of Biodegradable Multifunctional Nanoplatforms for Imaging‐Guided Brain Tumor Treatment

Chen

et al. 2018

Advanced Science

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“…These studies have shown that the BBB disruption (BBBD) lasts for a few hours (Hynynen et al 2001;Hynynen et al 2005;Hynynen et al 2006) and can be reliably applied with negligible damage to the brain parenchyma (Hynynen et al 2001;Hynynen et al 2005;McDannold et al 2005;Hynynen et al 2006), at least when compared to invasive techniques. Studies have also shown that the BBBD can be performed using low ultrasound frequencies (0.26 MHz and 0.69 MHz) suitable for trans-cranial application with a focused beam Hynynen et al 2006), and that delivery of chemotherapy (Treat et al 2005) and antibodies can be achieved (Kinoshita et al 2006b;Kinoshita et al 2006a). …”

Section: Introductionmentioning

confidence: 99%

Use of Ultrasound Pulses Combined with Definity for Targeted Blood-Brain Barrier Disruption: A Feasibility Study

McDannold

Vykhodtseva

Hynynen

2007

Ultrasound in Medicine & Biology

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129

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We have developed a method to use low-intensity focused ultrasound pulses combined with an ultrasound contrast agent to produce temporary blood-brain barrier disruption (BBBD). This method could provide a means for the targeted delivery of drugs or imaging agents into the brain. All of our previous work used Optison ® as the ultrasound contrast agent. The purpose of this work was to test the feasibility of using the contrast agent Definity ® for BBBD. Thirty-six non-overlapping locations were sonicated through a craniotomy in experiments in the brains of nine rabbits (4 locations per rabbit; US frequency: 0.69MHz, burst: 10ms, PRF: 1Hz, duration: 20s). The peak negative pressure amplitude ranged from 0.2-1.5 MPa. Eleven additional locations were sonicated using Optison ® at a pressure amplitude of 0.5 MPa. Definity ® and Optison ® dosages were those used clinically for ultrasound imaging: 10 and 50 μl/kg, respectively. The probability for BBBD (determined using MRI contrast agent enhancement) as a function of pressure amplitude was similar to that found earlier with Optison ® . For both agents, the probability was estimated to be 50% at 0.4 MPa using probit regression. Histological examination revealed small isolated areas of extravasated erythrocytes in some locations. At 0.8 MPa and above, this extravasation was sometimes accompanied by tiny (dimensions of 100 μm or less) regions of damaged brain parenchyma. The magnitude of the BBBD was larger with Optison ® than with Definity ® at 0.5 MPa (signal enhancement: 13.3 ± 4.4% vs. 8.4 ± 4.9%, P=0.04), and more areas with extravasated erythrocytes were observed with Optison ® (5.0 ± 3.5 vs. 1.4 ± 1.9 areas with extravasation in histology section with largest effect; P=0.03). We conclude that BBBD is possible using Definity ® for the dosage of contrast agent and the acoustic parameters tested in this study. While the probability for BBBD as a function of pressure amplitude and the type of acute tissue effects were similar to what has been observed with Optison ® , under these experimental conditions, Optison ® produced a larger effect for the same acoustic pressure amplitude.

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“…However, MRI contrast agents could be useful for monitoring. Studies investigating the delivery of chemotherapy agents (76) and antibodies (77,78) have found an association between the amount of agent delivered to the brain with the amount of contrast enhancement (Fig. 7).…”

Section: Bbb Openingmentioning

confidence: 98%

“…It can also be applied at frequencies suitable for a transcranial application (73,75). The focal, anatomically selective opening acts as a virtual needle that can be noninvasively used for any selected target, such as noninvasive targeted drug delivery (76,77). Examples of MRI showing focal BBB opening in a rabbit brain are shown in Fig.…”

Section: Bbb Openingmentioning

confidence: 99%

Current status and future potential of MRI‐guided focused ultrasound surgery

Jólesz

McDannold

2008

Magnetic Resonance Imaging

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112

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The combination of the imaging abilities of magnetic resonance imaging (MRI) with the ability to delivery energy to targets deep in the body noninvasively with focused ultrasound presents a disruptive technology with the potential to significantly affect healthcare. MRI offers precise targeting, visualization, and quantification of temperature changes and the ability to immediately evaluate the treatment. By exploiting different mechanisms, focused ultrasound offers a range of therapies, ranging from thermal ablation to targeted drug delivery. This article reviews recent preclinical and tests clinical of this technology. WHILE ITS POTENTIAL has been recognized for decades (1-4), focused ultrasound (FUS) therapy has been in the incubation phase for a long time. Although it has been tested in numerous animal experiments, its widespread clinical realization has lagged, primarily due to the lack of intraprocedural accurate temperature monitoring. When the idea of MRI-guidance was introduced in connection with FUS and MRI thermometry during sonication was demonstrated (5,6), it was anticipated that MR-guided FUS surgery (MRgFUS) would be widely accepted clinically within a few years. Despite these early expectations, there has been relatively slow progress in the clinical implementation of MRgFUS.Early development concentrated primarily on breast tumors (benign fibroadenoma (7,8) and malignant breast cancer (9,10)). These early implementations of the MRgFUS technology motivated the improvement of transducer technology from single-element transducers to MRI-compatible multielement phase arrays (11). There was also significant progress in MRI thermometry and its use to monitor and control sonications. Importantly, too, methods were developed to robustly quantify temperature changes (12). At first, only 2D temperature maps were obtained by MRI to allow for accurate targeting of the beam (13). Later these thermal images were used to generate maps of the thermal dose (14) that could then be used to tailor the energy deposition using closed-loop feedback control (15). This preclinical work led to the development of the first commercial system by InSightec (Haifa, Israel), the Exablate 2000, the first implementation of a fully integrated MRgFUS system that combined a phased array transducer, a computer-controlled robotic positioner, and a workstation that integrated control based on MR thermometry.The early limited clinical trials of breast tumor treatment (8 -10,16,17) were followed by the first major clinical application: the noninvasive therapy of benign uterine fibroids (18,19). The successful Phase I trial was followed by a multicenter . These clinical trials led to the approval of this technology for the treatment of uterine fibroids in several countries, including the United States. Examples of MR thermometry and postablation imaging of a uterine fibroid ablation are shown in Figure 1.The success of uterine fibroid ablation has invigorated the entire field. Technology has rapidly improved and clinical applications ke...

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Noninvasive localized delivery of Herceptin to the mouse brain by MRI-guided focused ultrasound-induced blood–brain barrier disruption

Cited by 582 publications

References 29 publications

Focused Ultrasound‐Augmented Delivery of Biodegradable Multifunctional Nanoplatforms for Imaging‐Guided Brain Tumor Treatment

Focused Ultrasound‐Augmented Delivery of Biodegradable Multifunctional Nanoplatforms for Imaging‐Guided Brain Tumor Treatment

Use of Ultrasound Pulses Combined with Definity for Targeted Blood-Brain Barrier Disruption: A Feasibility Study

Current status and future potential of MRI‐guided focused ultrasound surgery

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