接受剂量差异化加速放疗(DART - bid)治疗的患者中,与临床相关的急性食管炎(≥2级)的正常组织并发症模型。
Normal tissue complication models for clinically relevant acute esophagitis (≥ grade 2) in patients treated with dose differentiated accelerated radiotherapy (DART-bid).
作者信息
Zehentmayr Franz, Söhn Matthias, Exeli Ann-Katrin, Wurstbauer Karl, Tröller Almut, Deutschmann Heinz, Fastner Gerd, Fussl Christoph, Steininger Philipp, Kranzinger Manfred, Belka Claus, Studnicka Michael, Sedlmayer Felix
机构信息
Univ.-Klinik für Radiotherapie und Radio-Onkologie, Landeskrankenhaus Salzburg, Univ.-Klinikum der Paracelsus Medizinischen Privatuniversität, Müllner Hauptstr. 48, 5020, Salzburg, Austria.
Institute for Research and Development of Advanced Radiation Technologies (radART), Paracelsus Medizinische Privatuniversität, Müllner Hauptstr. 48, 5020, Salzburg, Austria.
出版信息
Radiat Oncol. 2015 May 28;10:121. doi: 10.1186/s13014-015-0429-1.
BACKGROUND
One of the primary dose-limiting toxicities during thoracic irradiation is acute esophagitis (AE). The aim of this study is to investigate dosimetric and clinical predictors for AE grade ≥ 2 in patients treated with accelerated radiotherapy for locally advanced non-small cell lung cancer (NSCLC).
PATIENTS AND METHODS
66 NSCLC patients were included in the present analysis: 4 stage II, 44 stage IIIA and 18 stage IIIB. All patients received induction chemotherapy followed by dose differentiated accelerated radiotherapy (DART-bid). Depending on size (mean of three perpendicular diameters) tumors were binned in four dose groups: <2.5 cm 73.8 Gy, 2.5-4.5 cm 79.2 Gy, 4.5-6 cm 84.6 Gy, >6 cm 90 Gy. Patients were treated in 3D target splitting technique. In order to estimate the normal tissue complication probability (NTCP), two Lyman models and the cutoff-logistic regression model were fitted to the data with AE ≥ grade 2 as statistical endpoint. Inter-model comparison was performed with the corrected Akaike information criterion (AICc), which calculates the model's quality of fit (likelihood value) in relation to its complexity (i.e. number of variables in the model) corrected by the number of patients in the dataset. Toxicity was documented prospectively according to RTOG.
RESULTS
The median follow up was 686 days (range 84-2921 days), 23/66 patients (35 %) experienced AE ≥ grade 2. The actuarial local control rates were 72.6 % and 59.4 % at 2 and 3 years, regional control was 91 % at both time points. The Lyman-MED model (D50 = 32.8 Gy, m = 0.48) and the cutoff dose model (Dc = 38 Gy) provide the most efficient fit to the current dataset. On multivariate analysis V38 (volume of the esophagus that receives 38 Gy or above, 95 %-CI 28.2-57.3) was the most significant predictor of AE ≥ grade 2 (HR = 1.05, CI 1.01-1.09, p = 0.007).
CONCLUSION
Following high-dose accelerated radiotherapy the rate of AE ≥ grade 2 is slightly lower than reported for concomitant radio-chemotherapy with the additional benefit of markedly increased loco-regional tumor control. In the current patient cohort the most significant predictor of AE was found to be V38. A second clinically useful parameter in treatment planning may be MED (mean esophageal dose).
背景
胸部放疗期间主要的剂量限制毒性之一是急性食管炎(AE)。本研究的目的是调查局部晚期非小细胞肺癌(NSCLC)患者接受加速放疗时AE≥2级的剂量学和临床预测因素。
患者与方法
本分析纳入66例NSCLC患者:4例II期、44例IIIA期和18例IIIB期。所有患者均接受诱导化疗,随后进行剂量区分加速放疗(DART-bid)。根据肿瘤大小(三个垂直直径的平均值)将肿瘤分为四个剂量组:<2.5 cm给予73.8 Gy,2.5 - 4.5 cm给予79.2 Gy,4.5 - 6 cm给予84.6 Gy,>6 cm给予90 Gy。患者采用三维靶区分割技术进行治疗。为了估计正常组织并发症概率(NTCP),将两个莱曼模型和截断逻辑回归模型拟合到以AE≥2级为统计终点的数据。使用校正的赤池信息准则(AICc)进行模型间比较,该准则根据数据集中患者数量校正后,计算模型相对于其复杂性(即模型中的变量数量)的拟合质量(似然值)。毒性按照RTOG前瞻性记录。
结果
中位随访时间为686天(范围84 - 2921天),23/66例患者(35%)发生AE≥2级。2年和3年的精算局部控制率分别为72.6%和59.4%,两个时间点的区域控制率均为91%。莱曼 - MED模型(D50 = 32.8 Gy,m = 0.48)和截断剂量模型(Dc = 38 Gy)对当前数据集的拟合效果最佳。多因素分析显示,V38(接受38 Gy及以上剂量的食管体积,95% - CI 28.2 - 57.3)是AE≥2级最显著的预测因素(HR = 1.05,CI 1.01 - 1.09,p = 0.007)。
结论
高剂量加速放疗后AE≥2级的发生率略低于同步放化疗报道的发生率,且具有局部区域肿瘤控制显著提高的额外益处。在当前患者队列中,发现AE最显著的预测因素是V38。治疗计划中另一个临床有用的参数可能是MED(平均食管剂量)。
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