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肺癌放疗:通过不对称准直进行靶区分割可减少对正常组织的辐射剂量并提高剂量。

Radiotherapy for lung cancer: target splitting by asymmetric collimation enables reduction of radiation doses to normal tissues and dose escalation.

作者信息

Wurstbauer K, Deutschmann H, Kranzinger M, Merz F, Rahim H, Sedlmayer F, Kogelnik H D

机构信息

Institute of Radiotherapy and Radio-Oncology, LKA Salzburg, Austria.

出版信息

Int J Radiat Oncol Biol Phys. 1999 May 1;44(2):333-41. doi: 10.1016/s0360-3016(99)00021-8.

Abstract

PURPOSE

This study was performed to develop a method of reducing the radiation doses to normal thoracic tissues, increasing the target dose, especially in the primary radiotherapy of non-small cell lung cancer (NSCLC), and to evaluate acute/subacute toxicity of dose escalation.

METHODS AND MATERIALS

From December 1195 to March 1998, the technique of target splitting has been applied to 58 patients. In this period, 30 patients were treated with doses > 80 Gy (ICRU-specification, mean 85.1 Gy, range 80. 1-90.2 Gy). The target volume is split into a cranial part (e.g., upper mediastinum) and a caudal part (e.g., primary tumor and middle mediastinum). Both volumes are planned and treated independently, using conformal irradiation techniques for both parts with half-collimated fields to prevent over- or underdosage in the junction plane. After fine-adjustment of the jaws, a verification film, exposed in a polymethylmethacrylate (PMMA) phantom, demonstrates the homogeneity of dose in the entire target volume. For comparison with conventional techniques, planning to identical doses is performed for 5 patients. Dose-volume histograms (DHVs) for normal lung tissue are presented for both methods.

RESULTS

The irradiated volume of normal tissue of the ipsilateral lung can be lowered at dose levels > or = 65, > or =45 Gy, and > or = 20 Gy to values of 37% (range 25-54%), 49% (range 46-54%), and 86% (range 55-117%), respectively. Other organs at risk, such as heart or esophagus, can also be spared significantly. Only 1 patient showed a transient grade 3 toxicity (pneumonitis), and there where no grade 4 acute/subacute side-effects. Two patients with Stage III A central tumors in close proximity to the large vessels died due to a pulmonary hemorrhage 2 and 4 months after therapy, respectively. No patient developed esophagitis. Antimycotic prophylaxis for esophagitis and posttherapeutic steroid prophylaxis for pneumonitis for several weeks were routinely used.

CONCLUSION

The technique of target splitting by asymmetric collimation helps to increase conformation, and thus enhances the sparing of normal tissues. It can be used whenever there is a marked difference in the shape of the planning target volume (PTV) in a cranio-caudal direction. This technique can principally be handled with 2D-planning systems, because it is coplanar. We consider target splitting as an important tool for dose escalation in the primary radiotherapy of NSCLC, that should also be used for other lung cancer patients necessitating moderate doses only.

摘要

目的

本研究旨在开发一种减少正常胸部组织辐射剂量、增加靶区剂量的方法,特别是在非小细胞肺癌(NSCLC)的初始放射治疗中,并评估剂量递增的急性/亚急性毒性。

方法与材料

从1995年12月至1998年3月,靶区分割技术应用于58例患者。在此期间,30例患者接受了大于80 Gy(ICRU规范,平均85.1 Gy,范围80.1 - 90.2 Gy)的剂量治疗。靶区体积被分割为头侧部分(如上纵隔)和尾侧部分(如原发肿瘤和中纵隔)。两个部分均独立进行计划和治疗,对两个部分均使用适形照射技术,采用半准直野以防止交界平面处剂量过高或过低。在精确调整准直器后,在聚甲基丙烯酸甲酯(PMMA)体模中曝光的验证片可显示整个靶区内剂量的均匀性。为与传统技术进行比较,对5例患者进行了相同剂量的计划。给出了两种方法的正常肺组织剂量 - 体积直方图(DVH)。

结果

同侧肺正常组织的受照体积在剂量水平≥65 Gy、≥45 Gy和≥20 Gy时可分别降低至37%(范围25% - 54%)、49%(范围46% - 54%)和86%(范围55% - 117%)。其他危及器官,如心脏或食管,也可得到显著保护。仅1例患者出现短暂的3级毒性(肺炎),未出现4级急性/亚急性副作用。两名患有ⅢA期中心型肿瘤且紧邻大血管的患者分别在治疗后2个月和4个月因肺出血死亡。无患者发生食管炎。常规使用抗真菌药物预防食管炎,并在数周内使用治疗后类固醇预防肺炎。

结论

通过不对称准直进行靶区分割的技术有助于提高适形性,从而增强对正常组织的保护。只要在头 - 尾方向上计划靶区体积(PTV)的形状存在显著差异,就可使用该技术。由于该技术是共面的,原则上可使用二维计划系统进行操作。我们认为靶区分割是NSCLC初始放射治疗中剂量递增的重要工具,也应用于仅需要中等剂量的其他肺癌患者。

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