首页> 外文期刊>Radiotherapy and oncology: Journal of the European Society for Therapeutic Radiology and Oncology >Sensitivity of treatment plan optimisation for prostate cancer using the equivalent uniform dose (EUD) with respect to the rectal wall volume parameter.
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Sensitivity of treatment plan optimisation for prostate cancer using the equivalent uniform dose (EUD) with respect to the rectal wall volume parameter.

机译:对于直肠壁体积参数,使用等效均匀剂量(EUD)对前列腺癌进行治疗计划优化的敏感性。

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BACKGROUND AND PURPOSE: To analyse the sensitivity of plan optimisation of prostate cancer treatments with respect to changes in the volume parameter (n), when the EUD is used to control the dose in the rectal wall. PATIENTS AND METHODS: A series of plans was defined, by varying n over a range between 0.08 and 1, and testing different cost functions and beam arrangements. In all cases, the aim was to minimise the EUD in the rectal wall, while ensuring specific dose coverage of the PTV, and limiting the dose in the other OARs. The results were evaluated in terms of 3-D dose distribution and with respect to the current clinical knowledge about late rectal toxicity after irradiation. RESULTS: Different values of n lead to very similar dose distributions over the PTV (differences in mean dose <1Gy, differences in dose given to 99% of the volume <1%). For the rectal wall, the following observations were made: (a) all cumulative DVH curves crossed each other around 60Gy; (b) the rectal wall volume receiving doses between 30 and 45Gy could change by 45 and 30%, respectively, depending on the value of n; (c) for doses higher than 70Gy the differences were typically within 5%. Different values of n also affected the position of isodose surfaces. The distance between the 70 and the 30Gy isodose curves changed in the AP direction by a factor of 3 when n decreased from 1 to 0.08. High values of n were associated with less dose conformity and a larger volume (at least 20%) of normal tissues receiving 50Gy or more. All DVHs for the rectal wall were below published dose toxicity thresholds except when the prescribed dose was escalated up to 86Gy. CONCLUSIONS: In most cases, the solutions associated with n values up to 0.25 produced similar dose distribution in the rectal wall for doses above 45Gy, complying with the dose-toxicity thresholds we analysed. The choice of a specific value of n in the optimisation requires an analysis of its effects on the dose distribution for the rectal wall, but also on other aspects, such as the value of the dose to the non-involved normal tissues.
机译:背景与目的:当使用EUD控制直肠壁剂量时,要分析前列腺癌治疗方案优化对体积参数(n)变化的敏感性。患者和方法:通过在0.08和1之间的范围内改变n并测试不同的成本函数和光束布置,定义了一系列计划。在所有情况下,目的都是在确保PTV的特定剂量覆盖率并限制其他OAR中的剂量的同时,尽量减少直肠壁的EUD。根据3-D剂量分布以及关于放射后晚期直肠毒性的当前临床知识对结果进行了评估。结果:不同的n值导致PTV上的剂量分布非常相似(平均剂量差异<1Gy,剂量差异99%的体积<1%)。对于直肠壁,进行了以下观察:(a)所有累积的DVH曲线在60Gy左右彼此交叉; (b)根据n的值,接受30至45Gy剂量的直肠壁容积可能分别改变45%和30%; (c)对于高于70Gy的剂量,差异通常在5%以内。 n的不同值也会影响等剂量面的位置。当n从1减小到0.08时,70和30Gy等剂量曲线之间的距离沿AP方向变化了3倍。 n的高值与剂量一致性较低和接受50Gy或更多剂量的正常组织的较大体积(至少20%)相关。直肠壁的所有DVH均低于公布的剂量毒性阈值,除非将处方剂量提高至86Gy。结论:在大多数情况下,对于大于45Gy的剂量,与n值高达0.25的溶液在直肠壁中产生相似的剂量分布,符合我们分析的剂量毒性阈值。在优化中选择特定的n值需要分析其对直肠壁剂量分布的影响,还需要分析其他方面,例如对未累及的正常组织的剂量值。

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