采用射野内观显示的大剂量胸部放疗在非小细胞肺癌中的应用结果:一项回顾性多因素分析
Results of high-dose thoracic irradiation incorporating beam's eye view display in non-small cell lung cancer: a retrospective multivariate analysis.
作者信息
Hazuka M B, Turrisi A T, Lutz S T, Martel M K, Ten Haken R K, Strawderman M, Borema P L, Lichter A S
机构信息
Department of Radiation Oncology, University of Michigan Medical Center, Ann Arbor 48109.
出版信息
Int J Radiat Oncol Biol Phys. 1993 Sep 30;27(2):273-84. doi: 10.1016/0360-3016(93)90238-q.
PURPOSE
To review the University of Michigan clinical experience in nonsmall cell lung cancer using high-dose thoracic irradiation (> or = 60 Gy) so that a starting dose for our prospective dose-escalation study could be determined.
METHODS AND MATERIALS
Eighty-eight consecutive patients diagnosed with medically inoperable or locally advanced, unresectable nonsmall cell lung cancer were identified who were treated with thoracic irradiation alone to a minimum total dose of 60 Gy (uncorrected for lung density). All patients except four (95%) underwent computed tomography scanning for treatment planning that included beam's eye view display for tumor and critical structure localization. All patients were treated with standard fractionation in a continuous course to uncorrected total doses ranging from 60 to 74 Gy (median, 67.6 Gy).
RESULTS
The median follow-up exceeds 24 months for all surviving patients (range, 12 to 78 months). The median survival time was 15 months, and the 2- and 3-year overall actuarial survival rates were 37% and 15%, respectively. Survival was significantly different between stage of disease (p = .004) and N-stage (p = .002) by univariate analysis. In a multivariate analysis, stage becomes the only characteristic significantly associated with outcome. The median time to local progression for 86 evaluable patients was 29 months. Stage (p = .0003), T-stage (p = .0095) and N-stage (p = .027) were significantly different with respect to local progression-free survival by univariate analysis. However, only stage was prognostic for local progression-free survival by multivariate analysis. There was no difference between large volume treatment (inclusion of the contralateral hilar and supraclavicular lymph nodes) and small volume treatment (exclusion of these elective nodal sites) with respect to local progression-free survival (p = .507) or survival (p = .520). With regard to dose, there was no significant difference between patients who received > 67.6 Gy and patients who received < or = 67.6 Gy with respect to local progression-free survival (p = .094) or survival (p = .142). Within the Stage III subgroup, local progression-free survival (p = .018) and survival (p = .061) were longer favoring the high-dose group of patients. Despite these doses, disease progression within the irradiated field was the predominant first site of treatment failure.
CONCLUSION
This retrospective study has shown that it is feasible to deliver uncorrected tumor doses as high as 70 Gy using standard fractionation in NSCLC with acceptable morbidity. Local control remains a significant problem. These data indicate justification for a starting dose in a prospective radiation dose-escalation study.
目的
回顾密歇根大学使用高剂量胸部照射(≥60 Gy)治疗非小细胞肺癌的临床经验,以便确定我们前瞻性剂量递增研究的起始剂量。
方法与材料
连续纳入88例诊断为医学上无法手术或局部晚期、不可切除的非小细胞肺癌患者,这些患者仅接受胸部照射,最小总剂量为60 Gy(未校正肺密度)。除4例患者外(95%),所有患者均接受计算机断层扫描以进行治疗计划,其中包括用于肿瘤和关键结构定位的射野方向观显示。所有患者均采用标准分割连续疗程,未校正的总剂量范围为60至74 Gy(中位数为67.6 Gy)。
结果
所有存活患者的中位随访时间超过24个月(范围为12至78个月)。中位生存时间为15个月,2年和3年的总精算生存率分别为37%和15%。单因素分析显示,疾病分期(p = 0.004)和N分期(p = 0.002)的生存率存在显著差异。多因素分析中,分期成为与预后显著相关的唯一特征。86例可评估患者的局部进展中位时间为29个月。单因素分析显示,分期(p = 0.0003)、T分期(p = 0.0095)和N分期(p = 0.027)在无局部进展生存期方面存在显著差异。然而,多因素分析中只有分期对无局部进展生存期具有预后意义。在无局部进展生存期(p = 0.507)或生存率(p = 0.520)方面,大体积治疗(包括对侧肺门和锁骨上淋巴结)与小体积治疗(排除这些选择性淋巴结部位)之间无差异。关于剂量,接受>67.6 Gy的患者与接受≤67.6 Gy的患者在无局部进展生存期(p = 0.094)或生存率(p = 0.142)方面无显著差异。在Ⅲ期亚组中,高剂量组患者的无局部进展生存期(p = 0.018)和生存率(p = 0.061)更长。尽管采用了这些剂量,照射野内的疾病进展仍是主要的首次治疗失败部位。
结论
这项回顾性研究表明,在非小细胞肺癌中使用标准分割给予高达70 Gy的未校正肿瘤剂量且发病率可接受是可行的。局部控制仍然是一个重大问题。这些数据为前瞻性放射剂量递增研究的起始剂量提供了依据。
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