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使用笔束算法和蒙特卡罗算法对剂量计算准确性进行定量评估以及临床质量保证要求。

Quantitative assessment of the accuracy of dose calculation using pencil beam and Monte Carlo algorithms and requirements for clinical quality assurance.

作者信息

Ali Imad, Ahmad Salahuddin

机构信息

Department of Radiation Oncology, University of Oklahoma Health Sciences Center, Oklahoma City, OK 73104, USA.

出版信息

Med Dosim. 2013 Autumn;38(3):255-61. doi: 10.1016/j.meddos.2013.02.005. Epub 2013 Apr 2.

DOI:10.1016/j.meddos.2013.02.005
PMID:23558145
Abstract

To compare the doses calculated using the BrainLAB pencil beam (PB) and Monte Carlo (MC) algorithms for tumors located in various sites including the lung and evaluate quality assurance procedures required for the verification of the accuracy of dose calculation. The dose-calculation accuracy of PB and MC was also assessed quantitatively with measurement using ionization chamber and Gafchromic films placed in solid water and heterogeneous phantoms. The dose was calculated using PB convolution and MC algorithms in the iPlan treatment planning system from BrainLAB. The dose calculation was performed on the patient's computed tomography images with lesions in various treatment sites including 5 lungs, 5 prostates, 4 brains, 2 head and necks, and 2 paraspinal tissues. A combination of conventional, conformal, and intensity-modulated radiation therapy plans was used in dose calculation. The leaf sequence from intensity-modulated radiation therapy plans or beam shapes from conformal plans and monitor units and other planning parameters calculated by the PB were identical for calculating dose with MC. Heterogeneity correction was considered in both PB and MC dose calculations. Dose-volume parameters such as V95 (volume covered by 95% of prescription dose), dose distributions, and gamma analysis were used to evaluate the calculated dose by PB and MC. The measured doses by ionization chamber and EBT GAFCHROMIC film in solid water and heterogeneous phantoms were used to quantitatively asses the accuracy of dose calculated by PB and MC. The dose-volume histograms and dose distributions calculated by PB and MC in the brain, prostate, paraspinal, and head and neck were in good agreement with one another (within 5%) and provided acceptable planning target volume coverage. However, dose distributions of the patients with lung cancer had large discrepancies. For a plan optimized with PB, the dose coverage was shown as clinically acceptable, whereas in reality, the MC showed a systematic lack of dose coverage. The dose calculated by PB for lung tumors was overestimated by up to 40%. An interesting feature that was observed is that despite large discrepancies in dose-volume histogram coverage of the planning target volume between PB and MC, the point doses at the isocenter (center of the lesions) calculated by both algorithms were within 7% even for lung cases. The dose distributions measured with EBT GAFCHROMIC films in heterogeneous phantoms showed large discrepancies of nearly 15% lower than PB at interfaces between heterogeneous media, where these lower doses measured by the film were in agreement with those by MC. The doses (V95) calculated by MC and PB agreed within 5% for treatment sites with small tissue heterogeneities such as the prostate, brain, head and neck, and paraspinal tumors. Considerable discrepancies, up to 40%, were observed in the dose-volume coverage between MC and PB in lung tumors, which may affect clinical outcomes. The discrepancies between MC and PB increased for 15MV compared with 6MV indicating the importance of implementation of accurate clinical treatment planning such as MC. The comparison of point doses is not representative of the discrepancies in dose coverage and might be misleading in evaluating the accuracy of dose calculation between PB and MC. Thus, the clinical quality assurance procedures required to verify the accuracy of dose calculation using PB and MC need to consider measurements of 2- and 3-dimensional dose distributions rather than a single point measurement using heterogeneous phantoms instead of homogenous water-equivalent phantoms.

摘要

比较使用BrainLAB铅笔束(PB)算法和蒙特卡罗(MC)算法计算位于包括肺部在内的不同部位肿瘤的剂量,并评估验证剂量计算准确性所需的质量保证程序。还使用放置在固体水和非均匀体模中的电离室和Gafchromic胶片进行测量,定量评估PB和MC的剂量计算准确性。使用BrainLAB的iPlan治疗计划系统中的PB卷积和MC算法计算剂量。在患者的计算机断层扫描图像上进行剂量计算,病变位于包括5个肺部、5个前列腺、4个脑部、2个头颈部和2个脊柱旁组织在内的各种治疗部位。剂量计算中使用了传统放疗、适形放疗和调强放疗计划的组合。在使用MC计算剂量时,调强放疗计划的叶片序列或适形计划的射束形状以及PB计算的监测单位和其他计划参数保持一致。PB和MC剂量计算中均考虑了不均匀性校正。使用V95(处方剂量的95%覆盖的体积)等剂量体积参数、剂量分布和伽马分析来评估PB和MC计算的剂量。在固体水和非均匀体模中使用电离室和EBT GAFCHROMIC胶片测量的剂量用于定量评估PB和MC计算剂量的准确性。PB和MC在脑部、前列腺、脊柱旁和头颈部计算的剂量体积直方图和剂量分布彼此吻合良好(在5%以内),并提供了可接受的计划靶体积覆盖。然而,肺癌患者的剂量分布存在较大差异。对于用PB优化的计划,剂量覆盖在临床上显示为可接受,而实际上,MC显示出系统性的剂量覆盖不足。PB计算的肺部肿瘤剂量高估了高达40%。观察到的一个有趣特征是,尽管PB和MC在计划靶体积的剂量体积直方图覆盖方面存在很大差异,但即使对于肺部病例来说,两种算法在等中心(病变中心)计算的点剂量也在7%以内。在非均匀体模中用EBT GAFCHROMIC胶片测量的剂量分布在非均匀介质之间的界面处显示出比PB低近15%的较大差异,胶片测量的这些较低剂量与MC测量的剂量一致。对于前列腺、脑、头颈部和脊柱旁肿瘤等组织不均匀性较小的治疗部位,MC和PB计算的剂量(V95)在5%以内吻合。在肺部肿瘤的剂量体积覆盖方面,MC和PB之间观察到高达40%的显著差异,这可能会影响临床结果。与6MV相比,15MV时MC和PB之间的差异增大,表明实施如MC这样准确的临床治疗计划的重要性。点剂量的比较不能代表剂量覆盖的差异,在评估PB和MC之间的剂量计算准确性时可能会产生误导。因此,验证使用PB和MC进行剂量计算准确性所需的临床质量保证程序需要考虑二维和三维剂量分布的测量,而不是使用非均匀体模而不是均匀水等效体模进行单点测量。

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