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螺旋断层放射治疗中呼吸相互作用效应的三维分析:基线变化导致了大部分所见的剂量不均匀性。

Three-dimensional analysis of the respiratory interplay effect in helical tomotherapy: Baseline variations cause the greater part of dose inhomogeneities seen.

作者信息

Tudor G Samuel J, Harden Susan V, Thomas Simon J

机构信息

Department of Medical Physics and Clinical Engineering, Cambridge University Hospitals NHS Foundation Trust, Box 152, Addenbrooke's Hospital, Hills Road, Cambridge CB2 0QQ, United Kingdom and Department of Oncology, Cambridge University, Cambridge CB2 0QQ, United Kingdom.

Oncology Centre, Cambridge University Hospitals NHS Foundation Trust, Box 192, Addenbrooke's Hospital, Hills Road, Cambridge CB2 0QQ, United Kingdom.

出版信息

Med Phys. 2014 Mar;41(3):031704. doi: 10.1118/1.4864241.

Abstract

PURPOSE

Dose differences from those planned can occur due to the respiratory interplay effect on helical tomotherapy. The authors present a technique to calculate single-fraction doses in three-dimensions resulting from craniocaudal motion applied to a patient CT set. The technique is applied to phantom and patient plans using patient respiratory traces. An additional purpose of the work is to determine the contribution toward the interplay effect of different components of the respiratory trace.

METHODS

MATLAB code used to calculate doses to a CT dataset from a helical tomotherapy plan has been modified to permit craniocaudal motion and improved temporal resolution. Real patient traces from seven patients were applied to ten phantom plans of differing field width, modulation factor, pitch and fraction dose, and simulations made with peak-to-peak amplitudes ranging from 0 to 2.5 cm. PTV voxels near the superior or inferior limits of the PTV are excluded from the analysis. The maximum dose discrepancy compared with the static case recorded along with the proportion of voxels receiving more than 10% and 20% different from prescription dose. The analysis was repeated with the baseline variation of the respiratory trace removed, leaving the cyclic component of motion only. Radiochromic film was used on one plan-trace combination and compared with the software simulation. For one case, filtered traces were generated and used in simulations which consisted only of frequencies near to particular characteristic frequencies of the treatment delivery. Intraslice standard deviation of dose differences was used to identify potential MLC interplay, which was confirmed using nonmodulated simulations. Software calculations were also conducted for four realistic patient plans and modeling movement of a patient CT set with amplitudes informed by the observed motion of the GTV on 4DCT.

RESULTS

The maximum magnitude of dose difference to a PTV voxel due to the interplay effect within a particular plan-trace combination for peak-to-peak amplitudes of up to 2.5 cm ranged from 4.5% to 51.6% (mean: 23.8%) of the dose delivered in the absence of respiratory motion. For cyclic motion only, the maximum dose differences in each combination ranged from 2.1% to 26.2% (mean: 9.2%). There is reasonable correspondence between an example of the phantom plan simulations and radiochromic film measurement. The filtered trace simulations revealed that frequencies close to the characteristic frequency of the jaw motion across the target were found to generate greater interplay effect than frequencies close to the gantry frequency or MLC motion. There was evidence of interplay between respiratory motion and MLC modulation, but this is small compared with the interplay between respiratory motion and jaw motion. For patient-plan simulations, dose discrepancies are seen of up to 9.0% for a patient with 0.3 cm peak-to-peak respiratory amplitude and up to 17.7% for a patient with 0.9 cm peak-to-peak amplitude. These values reduced to 1.3% and 6.5%, respectively, when only cyclic motion was considered.

CONCLUSIONS

Software has been developed to simulate craniocaudal respiratory motion in phantom and patient plans using real patient respiratory traces. Decomposition of the traces into baseline andcyclic components reveals that the large majority of the interplay effect seen with the full trace is due to baseline variation during treatment.

摘要

目的

由于螺旋断层放疗中呼吸相互作用效应,可能会出现与计划剂量的差异。作者提出了一种技术,用于计算应用于患者CT数据集的头脚方向运动所产生的三维单次分割剂量。该技术使用患者呼吸轨迹应用于体模和患者计划。这项工作的另一个目的是确定呼吸轨迹不同组成部分对相互作用效应的贡献。

方法

用于从螺旋断层放疗计划计算CT数据集剂量的MATLAB代码已被修改,以允许头脚方向运动并提高时间分辨率。来自7名患者的真实患者轨迹被应用于10个不同射野宽度、调制因子、螺距和分割剂量的体模计划,并进行了峰峰值幅度范围为0至2.5 cm的模拟。分析中排除了PTV上下限附近的PTV体素。记录与静态情况相比的最大剂量差异以及接受的剂量与处方剂量相差超过10%和20%的体素比例。在去除呼吸轨迹的基线变化,仅保留运动的周期性成分后重复该分析。在一个计划-轨迹组合上使用放射变色胶片,并与软件模拟进行比较。对于一个病例,生成滤波后的轨迹并用于仅由接近治疗投送特定特征频率的频率组成的模拟。使用剂量差异的层内标准差来识别潜在的MLC相互作用,并通过非调制模拟进行确认。还对四个真实患者计划进行了软件计算,并根据在4DCT上观察到的GTV运动为患者CT数据集建模运动幅度。

结果

对于峰峰值幅度高达2.5 cm的特定计划-轨迹组合,由于相互作用效应导致的PTV体素剂量差异的最大幅度为无呼吸运动时所给予剂量的4.5%至51.6%(平均:23.8%)。仅对于周期性运动,每个组合中的最大剂量差异范围为2.1%至26.2%(平均:9.2%)。体模计划模拟的一个示例与放射变色胶片测量之间存在合理的对应关系。滤波后的轨迹模拟显示,发现接近穿过靶区的颌运动特征频率的频率比接近机架频率或MLC运动的频率产生更大的相互作用效应。有证据表明呼吸运动与MLC调制之间存在相互作用,但与呼吸运动和颌运动之间的相互作用相比,这很小。对于患者计划模拟,峰峰值呼吸幅度为0.3 cm的患者剂量差异高达9.0%,峰峰值幅度为0.9 cm的患者剂量差异高达17.7%。当仅考虑周期性运动时,这些值分别降至1.3%和6.5%。

结论

已开发出软件,使用真实患者呼吸轨迹在体模和患者计划中模拟头脚方向的呼吸运动。将轨迹分解为基线和周期性成分表明,完整轨迹中看到的大部分相互作用效应是由于治疗期间的基线变化。

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