早期胸部放疗和预防性颅脑放疗联合治疗限制期小细胞肺癌减少转移和提高生存率。

S S Kamath, D L McCarley, R A Zlotecki
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引用次数: 7

摘要

为了验证早期并发与顺序胸腔放疗(TRT)和铂/依托泊苷化疗的相对疗效,我们对48例有限期小细胞肺癌患者进行了早期并发(29例)或顺序(19例)TRT和铂/依托泊苷化疗。疾病特异性预后变量和预防性颅脑照射(PCI)的作用也进行了分析。34名患者(71%)接受了45 Gy剂量的TRT,分为25组(范围30-55 Gy)。大多数患者(75%)接受4-6个周期的化疗。在完成TRT和化疗后达到完全缓解的27例患者中有21例接受了PCI治疗。中位随访时间为29.3个月(范围12-98个月)。通过单因素和多因素分析评估潜在预后意义的变量。所有患者的绝对生存率和无复发生存率在2年和5年分别为42%和35%和32%和31%。27例患者有36个失败部位。9例患者发生胸部复发,中枢神经系统(CNS)是最常见的远处衰竭部位(15例)。多因素分析表明:(a)早期并发TRT和化疗与化疗后序贯TRT和(b)疾病体积[小于或大于胸宽的三分之一]对生存率有显著预测作用(P=0.036和P=0.05)。疾病体积小于胸宽三分之一的患者胸廓疾病控制率为79%,而疾病体积大于胸宽三分之一的患者胸廓疾病控制率为36% (P=0.0009)。早期并发TRT和化疗导致远处转移的发生率显著降低(并发组为26%,序贯组为63%;P = 0.008)。在接受PCI治疗的患者中,中枢神经系统控制率为86%,而未接受PCI治疗的患者为56%。我们的研究结果表明:(a)与序贯治疗相比,早期并发TRT和铂/依托泊苷化疗可提高生存率;(b)对完全全身反应的患者进行PCI治疗可有效预防中枢神经系统复发。我们还得出结论,胸部疾病体积是局部控制和总生存的重要预后因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Decreased metastasis and improved survival with early thoracic radiotherapy and prophylactic cranial irradiation in combined-modality treatment of limited-stage small cell lung cancer.

In an attempt to verify the relative efficacy of early concurrent vs. sequential timing of thoracic radiotherapy (TRT) and platinum/etoposide chemotherapy, 48 patients with limited-stage small cell lung cancer treated with either early-concurrent (29 patients) or sequential (19 patients) TRT and platinum/etoposide chemotherapy were evaluated. Disease-specific prognostic variables and the role of prophylactic cranial irradiation (PCI) were also analyzed. Thirty-four patients (71%) received TRT to a dose of 45 Gy in 25 fractions (range, 30-55 Gy). Most patients (75%) received 4-6 cycles of chemotherapy. Twenty-one of 27 patients achieving a complete response after completion of TRT and chemotherapy received PCI. Median follow-up was 29.3 months (range, 12-98 months). Variables of potential prognostic significance were evaluated by both univariate and multivariate analysis. The absolute and relapse-free survival rates for all patients were 42% and 35% at 2 years and 32% and 31% at 5 years, respectively. Thirty-six sites of failure were observed in 27 patients. Thoracic recurrence occurred in nine patients, and the central nervous system (CNS) was the most common site of distant failure (15 patients). Multivariate analysis demonstrated that (a) early concurrent TRT and chemotherapy vs. chemotherapy followed by sequential TRT and (b) disease volume [less than or greater than one-third of the thoracic width] were significantly predictive for survival (P=0.036 and P=0.05, respectively). Rates of control of thoracic disease were 79% for patients with a disease volume less than one-third of the thoracic width vs. 36% for disease volumes greater than one-third of the thoracic width (P=0.0009). Early concurrent TRT and chemotherapy resulted in a significantly lower incidence of distant metastasis (26% for concurrent vs. 63% for sequential; P=0.008). In patients who received PCI, the CNS control rate was 86% vs. 56% in patients not treated with PCI. Our findings suggest that (a) treatment with early concurrent TRT and platinum/etoposide chemotherapy may improve survival when compared with sequential treatment and (b) PCI for patients with complete systemic responses is effective in preventing CNS recurrence. We also conclude that thoracic disease volume is a significant prognostic factor for both local control and overall survival.

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