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Time-resolved dose distributions to moving targets during volumetric modulated arc therapy with and without dynamic MLC tracking

机译:带有和不带有动态MLC跟踪的体积调制电弧治疗期间移动目标的时间分辨剂量分布

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Purpose: The highly conformal doses delivered by volumetric modulated arc therapy (VMAT) may be compromised by intrafraction target motion. Although dynamic multileaf collimator (DMLC) tracking can mitigate the dosimetric impact of motion on the accumulated dose, residual errors still exist. The purpose of this study was to investigate the temporal evolution of dose errors throughout VMAT treatments delivered with and without DMLC tracking. Methods: Tracking experiments were performed on a linear accelerator connected to prototype DMLC tracking software. A three-axis motion stage reproduced representative clinical trajectories of four lung tumors and four prostates. For each trajectory, two VMAT treatment plans (low and high modulation) were delivered with and without DMLC tracking as well as to a static phantom for reference. Dose distributions were measured continuously at 72 Hz using a dosimeter with biplanar diode arrays. During tracking, the MLC leaves were continuously refitted to the 3D target position measured by an electromagnetic transponder at 30 Hz. The dosimetric errors caused in the 32 motion experiments were quantified by a time-resolved 3%/3 mm γ-test. The erroneously exposed areas in treatment beam's eye view (BEV) caused by inadequate real-time MLC adaptation were calculated and compared with the time-resolved γ failure rates. Results: The transient γ failure rate was on average 16.8% without tracking and 5.3% with tracking. The γ failure rate correlated well with the erroneously exposed areas in BEV (mean of Pearson r = 0.83, p < 0.001). For the final accumulated doses, the mean γ failure rate was 17.9% without tracking and 1.0% with tracking. With tracking the transient dose errors tended to cancel out resulting in the low mean γ failure rate for the accumulated doses. Conclusions: Time-resolved measurements allow pinpointing of transient errors in dose during VMAT delivery as well as monitoring of erroneous dose evolution in key target positions. The erroneously exposed area in BEV was shown to be a good indicator of errors in the dose distribution during treatment delivery.
机译:目的:体积调制内电弧治疗(VMAT)所提供的高保形剂量可能会受到分数内目标运动的影响。尽管动态多叶准直仪(DMLC)跟踪可以减轻运动对累积剂量的剂量学影响,但仍然存在残留误差。这项研究的目的是调查在有和没有DMLC跟踪的情况下进行的整个VMAT治疗中剂量误差的时间演变。方法:跟踪实验是在连接原型DMLC跟踪软件的线性加速器上进行的。三轴运动阶段再现了四个肺肿瘤和四个前列腺的典型临床轨迹。对于每条轨迹,在有和没有DMLC跟踪的情况下,都会交付两个VMAT治疗计划(低调制和高调制),并提供给静态模型以供参考。使用具有双平面二极管阵列的剂量计在72 Hz下连续测量剂量分布。在跟踪过程中,将MLC叶片连续重新安装到30 Hz的电磁应答器测量的3D目标位置。在32个运动实验中引起的剂量误差通过时间分辨的3%/ 3 mmγ测试进行量化。计算了由于实时MLC自适应不足而导致的在治疗光束的视线(BEV)中错误暴露的区域,并将其与时间分辨的γ故障率进行了比较。结果:瞬态γ失效率平均为16.8%(无跟踪)和5.3%(有跟踪)。 γ失效率与BEV中错误暴露的区域密切相关(Pearson的平均值r = 0.83,p <0.001)。对于最终的累积剂量,平均γ失败率是17.9%(不跟踪)和1.0%(跟踪)。通过跟踪,瞬时剂量误差趋于抵消,从而导致累积剂量的平均γ故障率低。结论:时间分辨测量可以精确定位VMAT输送过程中的剂量瞬时误差,并可以监控关键目标位置的错误剂量演变。 BEV中错误暴露的区域显示出可以很好地指示治疗过程中剂量分布的误差。

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