Medical Physics
Volume 41, Issue 6Part32 p. 554-555
Fifty-sixth annual meeting of the American association of physicists in medicine

TH-C-17A-05: Cherenkov Excited Phosphorescence Oxygen (CEPhOx) Imaging During Multi-Beam Radiation Therapy

R Zhang

R Zhang

Dartmouth College, Hanover, NH

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R Holt

R Holt

Dartmouth College, Hanover, NH – New Hampshire

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T Esipova

T Esipova

University of Pennsylvania, Philadelphia, PA

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S Vinogradov

S Vinogradov

University of Pennsylvania, Philadelphia, PA

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D Gladstone

D Gladstone

Dartmouth-Hitchcock Medical Center, Hanover, City of Lebanon

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B Pogue

B Pogue

Dartmouth College, Hanover, NH

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First published: 29 May 2014
https://doi.org/10.1118/1.4889616

Abstract

Purpose:

Cherenkov radiation is created during external beam radiation therapy that can excite phosphorescence in tissue from oxygen-sensitive, bio-compatible probes. Utilizing the known spatial information of the treatment plan with directed multiple beam angles, Cherenkov Excited Phosphorescence Oxygen (CEPhOx) imaging was realized from the reconstructions of Cherenkov excited phosphorescence lifetime.

Methods:

Platinum(II)-G4 (PtG4) was used as the oxygen-sensitive phosphorescent probe and added to a oxygenated cylindrical liquid phantom with a oxygenated/deoxygenated cylindrical anomaly. Cherenkov excited phosphorescence was imaged using a time-gated ICCD camera temporallysynchronized to the LINAC pulse output. Lifetime reconstruction was carried out in NIRFAST software. Multiple angles of the incident radiation beam was combined with the location of the prescribed treatment volume (PTV) to improve the tomographic recovery as a function of location. The tissue partial pressure of oxygen (pO2) in the background and PTV was calculated based on the recovered lifetime distribution and Stern-Volmer equation. Additionally a simulation study was performed to examine the accuracy of this technique in the setting of a human brain tumor.

Results:

Region-based pO2 values in the oxygenated background and oxygenated/deoxygenated PTV were correctly recovered, with the deoxygenated anomaly (15.4 mmHg) easily distinguished from the oxygenated background (143 mmHg). The data acquisition time could be achieved within the normal irradiation time for a human fractionated plan. The simulations indicated that CEPhOx would be a sufficient to sample tumor pO2 sensing from tumors which are larger than 2cm in diameter or within 23mm depth from the surface.

Conclusion:

CEPhOx could be a novel imaging tool for pO2 assessment during external radiation beam therapy. It is minimally invasive and should work within the established treatment plan of radiation therapy with multiple beams in situations where tumor pO2 measurement is a pertinent radiotherapy efficiency and dosimetric need.