Physical validation of UF-RIPSA: A rapid in-clinic peak skin dose mapping algorithm for fluoroscopically guided interventions

David Borrego; Emily L Marshall; Trung Tran; Daniel A Siragusa; Wesley E Bolch

doi:10.1002/acm2.12312

Physical validation of UF-RIPSA: A rapid in-clinic peak skin dose mapping algorithm for fluoroscopically guided interventions

J Appl Clin Med Phys. 2018 May;19(3):343-350. doi: 10.1002/acm2.12312. Epub 2018 Mar 25.

Authors

David Borrego¹, Emily L Marshall¹, Trung Tran¹, Daniel A Siragusa², Wesley E Bolch¹

Affiliations

¹ J. Crayton Pruitt Family Department of Biomedical Engineering, University of Florida, Gainesville, FL, USA.
² Radiology, Division of Vascular Interventional Radiology, University of Florida, Jacksonville, FL, USA.

Abstract

Purpose: The purpose of this study was to experimentally validate UF-RIPSA, a rapid in-clinic peak skin dose mapping algorithm developed at the University of Florida using optically stimulated luminescent dosimeters (OSLDs) and tissue-equivalent phantoms.

Methods: The OSLDs used in this study were InLight^TM Nanodot dosimeters by Landauer, Inc. The OSLDs were exposed to nine different beam qualities while either free-in-air or on the surface of a tissue equivalent phantom. The irradiation of the OSLDs was then modeled using Monte Carlo techniques to derive correction factors between free-in-air exposures and more complex irradiation geometries. A grid of OSLDs on the surface of a tissue equivalent phantom was irradiated with two fluoroscopic x ray fields generated by the Siemens Artis zee bi-plane fluoroscopic unit. The location of each OSLD within the grid was noted and its dose reading compared with UF-RIPSA results.

Results: With the use of Monte Carlo correction factors, the OSLD's response under complex irradiation geometries can be predicted from its free-in-air response. The predicted values had a percent error of -8.7% to +3.2% with a predicted value that was on average 5% below the measured value. Agreement within 9% was observed between the values of the OSLDs and RIPSA when irradiated directly on the phantom and within 14% when the beam first traverses the tabletop and pad.

Conclusions: The UF-RIPSA only computes dose values to areas of irradiated skin determined to be directly within the x ray field since the algorithm is based upon ray tracing of the reported reference air kerma value, with subsequent corrections for air-to-tissue dose conversion, x ray backscatter, and table/pad attenuation. The UF-RIPSA algorithm thus does not include the dose contribution of scatter radiation from adjacent fields. Despite this limitation, UF-RIPSA is shown to be fairly robust when computing skin dose to patients undergoing fluoroscopically guided interventions.

Keywords: Monte Carlo simulation; computational phantoms; fluoroscopically guided interventions; optically stimulated luminescent dosimeters (OSLDs); patient skin dose.

Publication types

Validation Study

MeSH terms

Algorithms*
Calibration
Fluoroscopy / methods*
Humans
Monte Carlo Method*
Phantoms, Imaging*
Radiation Dosage
Scattering, Radiation
Skin / radiation effects*
X-Rays

Grants and funding

F31 CA159464/CA/NCI NIH HHS/United States