Focused ultrasound releases cancer drugs on target

2019 03 28 18 32 8782 Fus Fig3d Thumb

The ability of focused ultrasound to heat tissue enables a range of noninvasive therapies, such as tumor ablation, for example, or relief of essential tremor. Another application under investigation is the use of ultrasound to induce mild hyperthermia (heating by no more than 6° C) and trigger drug release from thermosensitive liposomal carriers, enabling targeted drug delivery to tumors.

There are, however, challenges in translating ultrasound-induced drug release from small-animal studies to clinical use, including identification of a suitable technique for monitoring the heating process. MRI thermometry can measure temperature in real-time, but its high costs limit widespread application. Implanted temperature sensors, meanwhile, are necessarily invasive and may increase risk to the patient, as well as limiting which patients can be monitored.

Now, a team from the University of Oxford has investigated the use of computational planning models to determine the focused ultrasound parameters required to release drugs from liposomes, without the need for real-time thermometry. Such an approach could make ultrasound-mediated targeted drug delivery more widely accessible and simpler to administer than techniques that employ MRI guidance.

Treatment planning, modeling, and example results from a 50-year-old man with diffuse multilobular hepatocellular carcinoma in segment VI. Axial F-18 FDG PET/CT images obtained one day before (left) and 17 days after (right) treatment. Total lesion glycolysis of target tumor (white arrows) decreased by 36.4%, whereas there was no substantial change over the volume of a similarly sized tumor that received drug but no focused ultrasound (black arrows). Color bar indicates standardized uptake value. Images courtesy of Michael Gray, PhD, et al, Radiology.Treatment planning, modeling, and example results from a 50-year-old man with diffuse multilobular hepatocellular carcinoma in segment VI. Axial F-18 FDG PET/CT images obtained one day before (left) and 17 days after (right) treatment. Total lesion glycolysis of target tumor (white arrows) decreased by 36.4%, whereas there was no substantial change over the volume of a similarly sized tumor that received drug but no focused ultrasound (black arrows). Color bar indicates standardized uptake value. Images courtesy of Michael Gray, PhD, et al, Radiology.

"A key objective in developing the planning model was to not only validate the safety and feasibility of noninvasively triggered drug delivery in oncology, but to do so in a way that would enable large-scale adoption and deployment of the technique if successful," explains first author Michael Gray, PhD, senior research fellow in Clinical Therapeutic Ultrasound. "We hypothesized that neither expensive nor invasive thermometry would be necessary for mild hyperthermia-based treatments employing noninvasive ultrasound for targeted heating."

Patient-specific models

The study, part of the Safety and feasibility of ultrasound-triggered targeted drug delivery of doxorubicin from thermosensitive liposomes in liver tumors (TARDOX) trial, included 10 participants with liver tumors who were treated using focused ultrasound to release the cancer drug doxorubicin from liposomes. For the first six patients (group 1), the researchers used an implanted sensor to monitor temperature during ultrasonic heating of target tumors. They treated the other four patients without real-time thermometry, in a step toward fully noninvasive therapy (Radiology, 15 January 2019).

Diagram showing the treatment concept. In the first six participants, target temperature was monitored with a thermometry device implanted through a coaxial needle; for the other four participants, no thermometry device was used. Image courtesy of Michael Gray, PhD, et al, Radiology.Diagram showing the treatment concept. In the first six participants, target temperature was monitored with a thermometry device implanted through a coaxial needle; for the other four participants, no thermometry device was used. Image courtesy of Michael Gray, PhD, et al, Radiology.

Gray and colleagues developed a model to create focused ultrasound treatment plans, using a combination of participant data and finite element calculations. For each patient, the model recommends treatment parameters and predicts the resulting temperature fields.

"Patient images were used to create a combined acoustic/thermal anatomical model of the patient and target tumor," Gray explained. "Based on segmentation of CT and MRI data, each tissue type and tissue layer was assigned specific acoustic and thermal properties to enable predictive modeling of acoustic propagation and ultrasound-mediated hyperthermia."

The calculated treatment parameters showed that the prescribed power scaled approximately with target depth. For seven patients in whom model predictions were available at the time of treatment, the differences between predicted and implemented powers (mean, 3.5 W) were not clinically significant relative to the power used (mean, 64 W). These results indicate that the model consistently provides settings that are safe and agree with those chosen in the presence of thermometry.

The team also retrospectively created models for the first three participants, who were treated before model availability. The largest prediction discrepancy was seen for a patient with a target nearly 5 cm deeper than any others. On the basis of thermometry, this treatment was substantially underpowered. The researchers note that using model-predicted settings (had they been available) should have improved target heating.

For the three group 1 participants with treatment volumes of 52 cm3 or less (about the size of a golf ball), measured treatment-averaged temperatures were within 0.1° C to 0.3° C of the model predictions. For participants with larger tumors, the prediction was 1.4° C to 1.7° C below the measured value, suggesting that the small sensor used was not a reliable indicator of the median temperature of larger targets.

Treatment response

To assess therapeutic response, the team imaged all participants before and after treatment using contrast-enhanced MRI and CT and also FDG-PET/CT. In the first patient, PET revealed a 36.4% reduction in total lesion glycolysis of the target tumor, whereas there was no substantial response in a similarly sized tumor that received drug but no focused ultrasound. In six of the 10 participants, partial responses were seen after just one treatment cycle.

Histologic and MRI data showed no evidence of thermal tissue ablation, confirming the safety of this procedure. There were no skin burns, off-target tissue damage, or other clinically significant adverse effects related to focused ultrasound. The researchers also found that the model-prescribed treatments resulted in similar levels of enhanced drug delivery with or without real-time thermometry.

The TARDOX trial team, taken on the day of first treatment. Image courtesy of Michael Gray, PhD.The TARDOX trial team, taken on the day of first treatment. Image courtesy of Michael Gray, PhD.

The team concluded that the study supports the feasibility and safety of using planning models to define treatment parameters for targeted hyperthermic drug delivery to liver tumors without real-time thermometry.

"We are currently working on several additional clinical applications for the techniques developed in TARDOX, and hope to begin another phase I trial in another indication in the next 12 months," Gray said. "We are also exploring ultrasound-enhanced drug delivery using cavitational rather than thermal ultrasound mechanisms and will be starting a first-in-man study of this approach over the course of 2020."

Tami Freeman is the medical and biophysics editor for Physics World.

© IOP Publishing Limited. Republished with permission from Physics World, a website that helps scientists working in academic and industrial research stay up to date with the latest breakthroughs in physics and interdisciplinary science.

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