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Geometric and dosimetric comparison of four intrafraction motion adaptation strategies for stereotactic liver radiotherapy

机译:四种型肝脏放射治疗四大动作适应策略的几何和剂量测定

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The accuracy of stereotactic body radiotherapy (SBRT) in the liver is limited by tumor motion. Selection of the most suitable motion mitigation strategy requires good understanding of the geometric and dosimetric consequences. This study compares the geometric and dosimetric accuracy of actually delivered respiratory gated SBRT treatments for 15 patients with liver tumors with three simulated alternative motion adaptation strategies. The simulated alternatives are MLC tracking, baseline shift adaptation by inter-field couch corrections and no intrafraction motion adaptation. The patients received electromagnetic transponder-guided respiratory gated IMRT or conformal treatments in three fractions with a 3-4 mm gating window around the full exhale position. The CTV-PTV margin was 5 mm axially and 7-10 mm cranio-caudally. The CTV and PTV were covered with 95% and 67% of the prescribed mean CTV dose, respectively. The time-resolved target position error during treatments with the four investigated motion adaptation strategies was used to calculate motion margins and the motion-induced reduction in CTV D-95 relative to the planned dose (Delta D-95). The mean (range) number of couch corrections per treatment session to compensate for tumor drift was 2.8 (0-7) with gating, 1.4 (0-5) with baseline shift adaptation, and zero for the other strategies. The motion margins were 3.5 mm (left-right), 9.4 mm (cranio-caudal) and 3.9 mm (anterior-posterior) without intrafraction motion adaptation, approximately half of that with baseline shift adaptation, and 1-2 mm with MLC tracking and gating. With 7 mm CC margins the mean (range) of Delta D-95 for the CTV was 8.1 (0.6-29.4)%-points (no intrafraction motion adaptation), 4.0 (0.4-13.3)%-points (baseline shift adaptation), 1.0 (0.3-2.2)%-points (MLC tracking) and 0.8 (0.1-1.8)%-points (gating). With 10 mm CC margins Delta D-95 was instead 4.8 (0.3-14.8)%-points (no intrafraction motion adaptation) and 2.9 (0.2-9.8)%-points (baseline shift adaptation). In conclusion, baseline shift adaptation can mitigate gross dose deficits without the requirement of real-time motion adaptation. MLC tracking and gating, however, more effectively ensure high similarity between planned and delivered doses.
机译:肝脏立体定位体放射疗法(SBRT)的准确性受肿瘤运动的限制。选择最合适的运动缓解策略需要良好地了解几何和单次后果。该研究比较了具有三种模拟替代运动适应策略的15例肝脏肿瘤患者实际呼吸门控SBRT治疗的几何和剂量精度。模拟替代品是MLC跟踪,通过场间沙发校正的基线变速设施,没有间接运动适应。患者在三个级分中接受电磁应答器引导呼吸呼吸呼吸的IMRT或共形处理,在全呼气位置周围有3-4mm翼窗。 CTV-PTV裕度轴向5毫米,粗毛缘5毫米。 CTV和PTV分别覆盖95%和67%的规定的平均CTV剂量。使用四种调查的运动适应策略处理期间的时间分辨的目标位置误差用于计算相对于计划剂量(Delta D-95)的CTV D-95的运动边距和运动诱导的降低。每次治疗会议的平均(范围)待补偿肿瘤漂移的平均校正数为2.8(0-7),门控,1.4(0-5),基线移位适应,为其他策略为零。运动边距为3.5毫米(左右),9.4毫米(Cranio-Caudal)和3.9毫米(前后)而不具有Intrefraction Motion适配,大约有基线变速适配的一半,并且MLC跟踪1-2毫米门控。对于7 mm CC余量,CTV的ΔD-95的平均值(范围)为8.1(0.6-29.4)% - 点(无伸缩运动适应),4.0(0.4-13.3)% - 点(基线移位适应), 1.0(0.3-2.2)% - 点(MLC跟踪)和0.8(0.1-1.8)% - 点(门控)。使用10 mm CC MARGINS DELTA D-95代替4.8(0.3-14.8)% - 点(无伸缩运动适应)和2.9(0.2-9.8)% - 点(基线移位适应)。总之,基线移位适应可以减轻毛重缺陷,而无需实时运动适应。然而,MLC跟踪和门控更有效地确保了计划和递送剂量之间的高相似性。

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