Abstract

BackgroundRadiation induced secondary cancers are a rare but severe late effect after breast conserving therapy. Intraoperative radiotherapy (IORT) is increasingly used during breast conserving surgery. The purpose of this analysis was to estimate secondary cancer risks after IORT compared to other modalities of breast radiotherapy (APBI - accelerated partial breast irradiation, EBRT - external beam radiotherapy).MethodsComputer-tomography scans of an anthropomorphic phantom were acquired with an INTRABEAM IORT applicator (diameter 4 cm) in the outer quadrant of the breast and transferred via DICOM to the treatment planning system. Ipsilateral breast, contralateral breast, ipsilateral lung, contralateral lung, spine and heart were contoured. An INTRABEAM source (50 kV) was defined with the tip of the drift tube at the center of the spherical applicator. A dose of 20 Gy at 0 mm depth from the applicator surface was prescribed for IORT and 34 Gy (5 days × 2 × 3.4 Gy) at 10 mm depth for APBI. For EBRT a total dose of 50 Gy in 2 Gy fractions was planned using two tangential fields with wedges. The mean and maximal doses, DVHs and volumes receiving more than 0.1 Gy and 4 Gy of organs at risk (OAR) were calculated and compared. The life time risk for secondary cancers was estimated according to NCRP report 116.ResultsIORT delivered the lowest maximal doses to contralateral breast (< 0.3 Gy), ipsilateral (1.8 Gy) and contralateral lung (< 0.3 Gy), heart (1 Gy) and spine (< 0.3 Gy). In comparison, maximal doses for APBI were 2-5 times higher. EBRT delivered a maximal dose of 10.4 Gy to the contralateral breast and 53 Gy to the ipsilateral lung. OAR volumes receiving more than 4 Gy were 0% for IORT, < 2% for APBI and up to 10% for EBRT (ipsilateral lung). The estimated risk for secondary cancer in the respective OAR is considerably lower after IORT and/or APBI as compared to EBRT.ConclusionsThe calculations for maximal doses and volumes of OAR suggest that the risk of secondary cancer induction after IORT is lower than compared to APBI and EBRT.

Highlights

  • Radiation induced secondary cancers are a rare but severe late effect after breast conserving therapy

  • The importance of secondary cancer risks after radiation therapy has been recognized by several international organizations, including the International Commission on Radiological Protection (ICRP), the National Council on Radiation Protection and Measurement (NCRP), and the American Association of Physicist in Medicine (AAPM)

  • There are large differences in the dose distributions and especially in the low doses regions delivered to the organs at risk (OAR)

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Summary

Introduction

Radiation induced secondary cancers are a rare but severe late effect after breast conserving therapy. Intraoperative radiotherapy (IORT) is increasingly used during breast conserving surgery. The purpose of this analysis was to estimate secondary cancer risks after IORT compared to other modalities of breast radiotherapy (APBI - accelerated partial breast irradiation, EBRT - external beam radiotherapy). Breast-conserving surgery (BCS) followed by external-beam whole-breast radiotherapy (EBRT) has become the standard of care in early breast cancer. The importance of secondary cancer risks after radiation therapy has been recognized by several international organizations, including the International Commission on Radiological Protection (ICRP), the National Council on Radiation Protection and Measurement (NCRP), and the American Association of Physicist in Medicine (AAPM). Organs located far from the tumor volume (out-of-field organs) are assumed to receive low doses of radiation and, are frequently ignored in treatment planning, even though it is well known that small radiation doses to these organs can induce secondary cancers as well [9,10]

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