在使用立体定向体放射治疗（SBRT）治疗非小细胞肺癌时，在定义内部靶体积[ITV]时使用的呼吸阶段数的剂量学影响。

Annals of lung cancer Pub Date : 2019-01-01 Epub Date: 2019-10-05

Von Darius Heard, Eftekhar Rajab Bolookat, Bradley Rauschenbach, Kate Martin, Jorge Gomez, Anurag K Singh, Harish Malhotra

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引用次数: 0

摘要

在对非小细胞肺癌（NSCLC）进行立体定向体放射治疗（SBRT）时，通常需要根据四维计算机断层扫描（4DCT）数据集的 10 个阶段中每个阶段的靶点分割生成内靶体积（ITV），这大大增加了剂量测定的工作量。本研究探讨了使用较少相位数来编制 ITV 以获得同等结果的可行性。对 25 例接受 SBRT 治疗的肺癌患者进行了回顾性评估。患者按GTV在不同肺叶内的解剖位置分类，每叶5例。放射肿瘤专家在一个完整呼吸周期的 10 个不同阶段对 10 个 GTV 进行了轮廓分析。五个样本（样本 1-5）分别采用（0%、20%、40%、60%、80%，即每隔一个阶段）、（0%、30%、60%、90%，即跳过两个连续阶段）、（0%、20%、30%、50%，即基本上采用吸气、呼气和吸气阶段）、（0%、20%、40%、60%、80%，即每隔一个阶段）、（0%、30%、60%、90%，即跳过两个连续阶段）、（0%、20%、30%、50%，即基本上采用吸气、呼气和吸气阶段）。0%、30%、60%、90%，即跳过两个连续的阶段）、（0%、20%、30%、50%，即基本上使用吸气、呼气和中间的一个阶段）、（0%、30%、60%）、（0%、50%，即只完全使用吸气和呼气阶段）阶段 GTV，0% 被指定为吸气最多的阶段，50% 被指定为呼气最多的阶段。适当的样本 ITV 和 PTV 是以与临床计划相同的方式创建的，然后根据每套样本进行调整，修改幅度最小。将样本计划与临床治疗计划的等效剂量覆盖范围、质量中心和 ITV/PTV 容积差异进行比较。在控制呼吸的条件下，与临床 ITV 相比，平均 ITV 低估率从样本 1（0%、20%、40%、60%、80%）的最低 7.3% 增加到样本 5（0% 和 50%）的最高 24.5%。其他样本中也出现了类似的趋势，随着阶段数的减少，ITV/PTV 体积的低估率也在增加，与肿瘤位置无关。ITV 质量中心的平均变化极小（0.43 ± 0.11 毫米）。在使用少于全部 10 个阶段的 ITV/PTV 组合时，样本 1 和样本 5 的临床 PTV 剂量不足的最大值分别为 5.9% 和 12.3%。如果在生成 ITV 时使用的相位较少，则可能需要更大的 ITV 至 PTV 间隙才能获得同等的 PTV 覆盖率。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Dosimetric Implications of Number of Breathing Phases Used in the Definition of Internal Target Volume [ITV] in the Treatment of Non-Small Cell Lung Cancers Using Stereotactic Body Radiation Therapy (SBRT).

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Determination of intrafraction motion in stereotactic body radiation therapy (SBRT) of non-small-cell lung cancer (NSCLC) usually involves generating an internal target volume (ITV) based on target segmentation in every one of the 10 phases of a 4-dimensional computed tomography (4DCT) dataset which increases dosimetry work load substantially. This study explores the feasibility of using a smaller number of phases to compile an ITV to get equivalent results. Twenty-five lung cancer patients treated with SBRT were retrospectively assessed. Patients were categorized by the anatomic location of the GTV within different lobes of the lungs, 5 in each lobe. Ten GTVs were contoured by the radiation oncologist in 10 different phases of one complete respiratory cycle. Five samples (Sample 1-5) were created using (0%, 20%, 40%, 60%, 80% i.e. taking every other phase), (0%, 30%, 60%, 90% i.e. skipping two successive phases), (0%, 20%, 30%, 50% i.e. essentially taking inhale, exhale & a phase in between), (0%, 30%, 60%), (0%, 50% i.e. using completely inhale and exhale phase only) phase GTVs, 0% is designated as the most inhaled phase and 50% as the most exhaled phase. Appropriate sample ITVs and PTVs were created in the same manner as the clinical plan which was then adapted to each sample set with minimal modification. Sample plans were compared for equivalent dose coverage, center of mass, and ITV/PTV volume differences against the clinical treatment plan. The average % ITV underestimation against the clinical ITV increased from a minimum of 7.3% in sample 1 (0%, 20%, 40%, 60%, 80%) to a maximum of 24.5% in sample 5 (0% & 50%) under the conditions of controlled breathing. A similar trend was seen in other samples with the underestimation in the ITV/PTV volume increasing with the decrease in the number of phases irrespective of the tumor location. The average variation in the center of mass of the ITV was minimal (0.43 ± 0.11 mm). Use of ITV/PTV combination derived from using less than all 10 phases resulted in the maximum clinical PTV under-dosage of 5.9% for sample 1 and 12.3% for sample 5, respectively. If fewer phases in the generation of ITV are used, a larger ITV-to-PTV margin might be necessary to get equivalent PTV coverage.

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Annals of lung cancer

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