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根据对头颈部癌患者进行加速超分割放疗(CHART)或传统放疗后与治疗相关的发病率观察结果估算的修复半衰期。

Repair halftimes estimated from observations of treatment-related morbidity after CHART or conventional radiotherapy in head and neck cancer.

作者信息

Bentzen S M, Saunders M I, Dische S

机构信息

Gray Laboratory Cancer Research Trust and the Cancer Centre, Mount Vernon Hospital, Northwood, Middlesex, UK.

出版信息

Radiother Oncol. 1999 Dec;53(3):219-26. doi: 10.1016/s0167-8140(99)00151-6.

Abstract

BACKGROUND AND PURPOSE

The CHART (Continuous Hyperfractionated Accelerated Radiotherapy) head and neck cancer fractionation schedule delivered 54 Gy in 36 fractions on 12 consecutive days and this was compared in a randomised controlled trial with conventional fractionation delivering 66 Gy in 33 fractions over 6-7 weeks. Patients receiving CHART experienced statistically significantly less treatment-related morbidity after 6 months than patients receiving conventional fractionation. However, this improved tolerance was much less than anticipated from existing knowledge of dose-fractionation effects on late-responding normal tissues. Here, the experience from the CHART study is analysed and repair halftimes for three types of late treatment-related morbidity of human tissues are estimated.

PATIENTS AND METHODS

The CHART trial was open for patient accrual from March 1990 to April 1995 and a total of 918 patients in 11 participating centres were randomised. All patients were followed at regular intervals for a minimum of 5 years or until the time of death. At each follow-up, a number of treatment-related morbidity items were evaluated and scored prospectively. Data for three late endpoints are analysed here: laryngeal oedema, skin telangiectasia and subcutaneous fibrosis. Differences in the incidence of these endpoints in the two trial arms were quantified by means of the ratio of hazard rates in a Cox proportional hazards model. Monte Carlo sampling was performed from distributions of fractionation sensitivity (quantified by the alpha/beta-ratio) and steepness of the dose-response curve (quantified by the normalised dose-response gradient, gamma50) with means and standard deviations derived from the literature. Each pair of values were used to convert a Monte Carlo sampled estimate of the difference in biological effect into an estimate of the repair halftime. From the distribution of 1000 Monte Carlo samples, the mean repair halftime and its 95% confidence interval were estimated.

RESULTS

The estimated repair halftimes, with 95% confidence intervals in parentheses, were 4.9 h (3.2, 6.4) for laryngeal oedema, 3.8 h (2.5, 4.6) for skin telangiectasia and 4.4 h (3.8, 4.9) for subcutaneous fibrosis. Calculations show that these repair halftimes are consistent with the observations from two published randomised controlled trials of altered fractionation in head and neck cancer, the EORTC 22791 and 22851 trials.

CONCLUSIONS

These long repair halftimes for late effects in human normal tissues have to be considered in order to gain the full benefit from fractionation schedules employing multiple fractions per day.

摘要

背景与目的

CHART(持续超分割加速放疗)头颈癌分割方案在连续12天内分36次给予54 Gy剂量,并在一项随机对照试验中与传统分割方案进行比较,传统分割方案在6 - 7周内分33次给予66 Gy剂量。接受CHART方案治疗的患者在6个月后与接受传统分割方案的患者相比,治疗相关的发病率在统计学上显著更低。然而,这种耐受性的改善远低于根据现有关于剂量分割对晚期反应正常组织影响的知识所预期的程度。在此,对CHART研究的经验进行分析,并估计人体组织三种晚期治疗相关发病率的修复半衰期。

患者与方法

CHART试验于1990年3月至1995年4月开放招募患者,11个参与中心的918例患者被随机分组。所有患者定期随访至少5年或直至死亡。每次随访时,前瞻性地评估和记录多项治疗相关的发病情况并进行评分。这里分析三个晚期终点的数据:喉水肿、皮肤毛细血管扩张和皮下纤维化。通过Cox比例风险模型中的风险率之比来量化两个试验组中这些终点发生率的差异。根据文献得出的均值和标准差,从分割敏感性分布(通过α/β比值量化)和剂量反应曲线的陡峭程度(通过归一化剂量反应梯度γ50量化)进行蒙特卡罗抽样。每对数值用于将生物效应差异的蒙特卡罗抽样估计值转换为修复半衰期的估计值。从1000次蒙特卡罗抽样的分布中,估计平均修复半衰期及其95%置信区间。

结果

估计的修复半衰期(括号内为95%置信区间),喉水肿为4.9小时(3.2,6.4),皮肤毛细血管扩张为3.8小时(2.5,4.6),皮下纤维化为4.4小时(3.8,4.9)。计算表明,这些修复半衰期与两项已发表的头颈癌分割方案改变的随机对照试验(EORTC 22791和22851试验)的观察结果一致。

结论

为了从每天多次分割的分割方案中充分获益,必须考虑人体正常组织晚期效应的这些长修复半衰期。

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