Abstract

Cherenkov-excited luminescence scanned imaging (CELSI) is achieved with external beam radiotherapy to map out molecular luminescence intensity or lifetime in tissue. Just as in fluorescence microscopy, the choice of excitation geometry can affect the imaging time, spatial resolution and contrast recovered. In this study, the use of spatially patterned illumination was systematically studied comparing scan shapes, starting with line scan and block patterns and increasing from single beams to multiple parallel beams and then to clinically used treatment plans for radiation therapy. The image recovery was improved by a spatial-temporal modulation-demodulation method, which used the ability to capture simultaneous images of the excitation Cherenkov beam shape to deconvolve the CELSI images. Experimental studies used the multi-leaf collimator on a clinical linear accelerator (LINAC) to create the scanning patterns, and image resolution and contrast recovery were tested at different depths of tissue phantom material. As hypothesized, the smallest illumination squares achieved optimal resolution, but at the cost of lower signal and slower imaging time. Having larger excitation blocks provided superior signal but at the cost of increased radiation dose and lower resolution. Increasing the scan beams to multiple block patterns improved the performance in terms of image fidelity, lower radiation dose and faster acquisition. The spatial resolution was mostly dependent upon pixel area with an optimized side length near 38mm and a beam scan pitch of P = 0.33, and the achievable imaging depth was increased from 14mm to 18mm with sufficient resolving power for 1mm sized test objects. As a proof-of-concept, in-vivo tumor mouse imaging was performed to show 3D rendering and quantification of tissue pO2 with values of 5.6mmHg in a tumor and 77mmHg in normal tissue.

Highlights

  • Radiation therapy induces Cherenkov light emission within tissue, and this signal provides potential for direct molecular sampling of the tissue microenvironment [1,2,3,4]

  • Since tissue partial pressure of oxygen is well known to affect the efficacy of radiotherapy [1,8,9], imaging this signal has been a primary focus of previous Cherenkov Excited Luminescence Scanned Imaging (CELSI) studies

  • An improvement to the line-scan methods would be multi-direction scanning, which could render a full-direction resolution enhancement, this would come at the cost of doubling the radiation dose and acquisition time

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Summary

Introduction

Radiation therapy induces Cherenkov light emission within tissue, and this signal provides potential for direct molecular sampling of the tissue microenvironment [1,2,3,4]. CELSI can provide threedimensional luminescence images through layer-scanned Cherenkov light sheet, which is carried out by movements of the multi leaf collimator (MLC) on the linear accelerator (LINAC), which is commonly used to provide conformal shaping of radiotherapy treatment beams [7]. This application has been experimentally demonstrated in-vivo and is hopeful for clinical trial use, taking advantage of the dynamics already inherent in radiotherapy treatments [5,6]. It might be possible that existing clinical treatment plans allow for high resolution imaging

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