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Dosimetric feasibility of an anthropomorphic three-dimensional PRESAGE® dosimeter for verification of single entry hybrid catheter accelerated partial breast brachytherapy

Published online by Cambridge University Press:  20 July 2018

Khalid Iqbal*
Affiliation:
Department of Radiation Physics, The University of Texas MD Anderson Cancer Center, Houston, TX, USA Department of Physics, The Islamia University, Bahawalpur, Pakistan Department of Radiation Oncology, Shaukat Khanum Cancer Hospital & Research Center, Lahore, Pakistan
Geoffrey S. Ibbott
Affiliation:
Department of Radiation Physics, The University of Texas MD Anderson Cancer Center, Houston, TX, USA
Ryan G. Lafratta
Affiliation:
Department of Radiation Physics, The University of Texas MD Anderson Cancer Center, Houston, TX, USA
Kent A. Gifford
Affiliation:
Department of Radiation Physics, The University of Texas MD Anderson Cancer Center, Houston, TX, USA
Muhammad Akram
Affiliation:
Department of Physics, The Islamia University, Bahawalpur, Pakistan
Saeed A. Buzdar
Affiliation:
Department of Physics, The Islamia University, Bahawalpur, Pakistan
*
Author for correspondence: Khalid Iqbal, Department Radiation Physics, The University of Texas MD Anderson Cancer Center, Houston, TX, USA. Tel: +924235905000. Fax: +924235945206. E-mail: khalid_phy@yahoo.com

Abstract

Purpose

To determine the feasibility of an anthropomorphic breast polyurethane-based three-dimensional (3D) dosimeter with cavity to measure dose distributions and skin dose for a commercial strut-based applicator strut-adjusted volume implant (SAVI™) 6–1.

Materials and methods

An anthropomorphic breast 3D dosimeter was created with a cavity to accommodate the SAVI™ strut-based device. 2 Gy was prescribed to the breast dosimeter having D95 to planning target volume evaluation (PTV_EVAL) while limiting 125% of the prescribed dose to the skin. Independent dose distribution verification was performed with GAFCHROMIC® EBT2 film. The dose distribution from the 3D dosimeter was compared to the distributions from commercial brachytherapy treatment planning system (TPS) and film. Point skin doses, line profiles and dose–volume histogram (DVHs) for the skin and PTV_EVAL were compared.

Results

The maximum difference in skin dose for TPS and the 3D dosimeter was 4% whereas 41% between the TPS and EBT2 film. The maximum dose difference for line profiles between TPS, 3D dosimeter, and film was 4·1%. DVHs of skin and PTV_EVAL for TPS and 3D dosimeter differed by a maximum of 4% at 5 mm depth and skin differed by a maximum 1·5% between TPS and 3D dosimeter. The criterion for gamma analysis comparison was 92·5% at ±5%±3 mm criterion. The TPS demonstrated at least ±5% comparability in predicting dose to the skin, PTV_EVAL and normal breast tissue.

Conclusions

3D anthropomorphic polyurethane dosimeter with cavity gives comparable results to the TPS dose predictions and GAFCHROMIC® EBT2 film results in the context of HDR brachytherapy.

Type
Original Article
Copyright
© Cambridge University Press 2018 

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