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使用门静脉剂量测定法进行三维心脏剂量重建,以估计乳腺癌放疗后正常组织并发症概率。

Three-dimensional heart dose reconstruction to estimate normal tissue complication probability after breast irradiation using portal dosimetry.

作者信息

Louwe R J W, Wendling M, van Herk M B, Mijnheer B J

机构信息

Department of Radiation Oncology, The Netherlands Cancer Institute/Antoni van Leeuwenhoek Hospital, Amsterdam, The Netherlands.

出版信息

Med Phys. 2007 Apr;34(4):1354-63. doi: 10.1118/1.2713216.

Abstract

Irradiation of the heart is one of the major concerns during radiotherapy of breast cancer. Three-dimensional (3D) treatment planning would therefore be useful but cannot always be performed for left-sided breast treatments, because CT data may not be available. However, even if 3D dose calculations are available and an estimate of the normal tissue damage can be made, uncertainties in patient positioning may significantly influence the heart dose during treatment. Therefore, 3D reconstruction of the actual heart dose during breast cancer treatment using electronic imaging portal device (EPID) dosimetry has been investigated. A previously described method to reconstruct the dose in the patient from treatment portal images at the radiological midsurface was used in combination with a simple geometrical model of the irradiated heart volume to enable calculation of dose-volume histograms (DVHs), to independently verify this aspect of the treatment without using 3D data from a planning CT scan. To investigate the accuracy of our method, the DVHs obtained with full 3D treatment planning system (TPS) calculations and those obtained after resampling the TPS dose in the radiological midsurface were compared for fifteen breast cancer patients for whom CT data were available. In addition, EPID dosimetry as well as 3D dose calculations using our TPS, film dosimetry, and ionization chamber measurements were performed in an anthropomorphic phantom. It was found that the dose reconstructed using EPID dosimetry and the dose calculated with the TPS agreed within 1.5% in the lung/heart region. The dose-volume histograms obtained with EPID dosimetry were used to estimate the normal tissue complication probability (NTCP) for late excess cardiac mortality. Although the accuracy of these NTCP calculations might be limited due to the uncertainty in the NTCP model, in combination with our portal dosimetry approach it allows incorporation of the actual heart dose. For the anthropomorphic phantom, and for fifteen patients for whom CT data were available to test our method, the average difference between the NTCP values obtained with our method and those resulting from the dose distributions calculated with the TPS was 0.1% +/- 0.3% (1 SD). Most NTCP values were 1%-2% lower than those obtained using the method described by Hurkmans et al. [Radiother. Oncol. 62, 163-171 (2002)], using the maximum heart distance determined from a simulator image as a single pre-treatment parameter. A similar difference between the two methods was found for twelve patients using in vivo EPID dosimetry; the average NTCP value obtained with EPID dosimetry was 0.9%, whereas an average NTCP value of 2.2% was derived using the method of Hurkmans et al. The results obtained in this study show that EPID dosimetry is well suited for in vivo verification of the heart dose during breast cancer treatment, and can be used to estimate the NTCP for late excess cardiac mortality. To the best of our knowledge, this is the first study using portal dosimetry to calculate a DVH and NTCP of an organ at risk.

摘要

心脏受照射是乳腺癌放疗期间的主要关注点之一。因此,三维(3D)治疗计划会很有用,但对于左侧乳腺癌治疗,由于可能无法获取CT数据,所以不一定总能实施。然而,即便有3D剂量计算且能对正常组织损伤进行估计,患者定位的不确定性在治疗期间仍可能显著影响心脏剂量。因此,人们研究了使用电子成像射野影像装置(EPID)剂量测定法对乳腺癌治疗期间实际心脏剂量进行3D重建。一种先前描述的从放射学中位面的治疗射野图像重建患者体内剂量的方法,与受照射心脏体积的简单几何模型相结合,以计算剂量体积直方图(DVH),从而在不使用计划CT扫描的3D数据的情况下独立验证治疗的这一方面。为研究我们方法的准确性,对15例有CT数据的乳腺癌患者,比较了通过完整3D治疗计划系统(TPS)计算得到的DVH和在放射学中位面重新采样TPS剂量后得到的DVH。此外,在一个人体模型中进行了EPID剂量测定以及使用我们的TPS进行的3D剂量计算、胶片剂量测定和电离室测量。结果发现,使用EPID剂量测定法重建的剂量与TPS计算的剂量在肺/心脏区域内相差1.5%以内。用EPID剂量测定法得到的剂量体积直方图用于估计晚期心脏额外死亡率的正常组织并发症概率(NTCP)。尽管由于NTCP模型的不确定性,这些NTCP计算的准确性可能有限,但结合我们的射野剂量测定方法,它能够纳入实际心脏剂量。对于人体模型以及15例有CT数据用于测试我们方法的患者,我们的方法得到的NTCP值与TPS计算的剂量分布得到的NTCP值之间的平均差异为0.1%±0.3%(1个标准差)。大多数NTCP值比使用Hurkmans等人[《放射肿瘤学》62, 163 - 171(2002)]描述的方法得到的值低1% - 2%,后者使用从模拟图像确定的最大心脏距离作为单一治疗前参数。对于12例使用体内EPID剂量测定法的患者,两种方法也发现了类似差异;用EPID剂量测定法得到的平均NTCP值为0.9%,而使用Hurkmans等人的方法得到的平均NTCP值为2.2%。本研究获得的结果表明,EPID剂量测定法非常适合在乳腺癌治疗期间对心脏剂量进行体内验证,并且可用于估计晚期心脏额外死亡率的NTCP。据我们所知,这是第一项使用射野剂量测定法计算危险器官的DVH和NTCP的研究。

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