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连续低剂量率照射和分次高剂量率照射的放射生物学方面

Radiobiological aspects of continuous low dose-rate irradiation and fractionated high dose-rate irradiation.

作者信息

Turesson I

机构信息

Department of Oncology, University of Gothenburg, Sweden.

出版信息

Radiother Oncol. 1990 Sep;19(1):1-15. doi: 10.1016/0167-8140(90)90161-o.

Abstract

The biological effects of continuous low dose-rate irradiation and fractionated high dose-rate irradiation in interstitial and intracavitary radiotherapy and total body irradiation are discussed in terms of dose-rate fractionation sensitivity for various tissues. A scaling between dose rate and fraction size was established for acute and late normal-tissue effects which can serve as a guideline for local treatment in the range of dose rates between 0.02 and 0.005 Gy/min and fraction sizes between 8.5 and 2.5 Gy. This is valid provided cell-cycle progression and proliferation can be ignored. Assuming that the acute and late tissue responses are characterised by alpha/beta values of about 10 and 3 Gy and a mono-exponential repair half-time of about 3 h, the same total doses given with either of the two methods are approximately equivalent. The equivalence for acute and late non-hemopoietic normal tissue damage is 0.02 Gy/min and 8.5 Gy per fraction; 0.01 Gy/min and 5.5 Gy per fraction; and 0.005 Gy/min and 2.5 Gy per fraction. A very low dose rate, below 0.005 Gy/min, is thus necessary to simulate high dose-rate radiotherapy with fraction sizes of about 2 Gy. The scaling factor is, however, dependent on the repair half-time of the tissue. A review of published data on dose-rate effects for normal-tissue response showed a significantly stronger dose-rate dependence for late than for acute effects below 0.02 Gy/min. There was no significant difference in dose-rate dependence between various acute non-hemopoietic effects or between various late effects. The consistent dose-rate dependence, which justifies the use of a general scaling factor between fraction size and dose rate, contrasts with the wide range of values for repair half-time calculated for various normal-tissue effects. This indicates that the model currently used for repair kinetics is not satisfactory. There are also few experimental data in the clinical dose-rate range, below 0.02 Gy/min. It is therefore necessary to verify further the presented scaling between fraction size and dose rate.

摘要

从不同组织的剂量率分割敏感性方面,讨论了连续低剂量率照射和分次高剂量率照射在组织间和腔内放疗以及全身照射中的生物学效应。针对急性和晚期正常组织效应,建立了剂量率与分次剂量之间的比例关系,这可作为剂量率在0.02至0.005 Gy/min之间且分次剂量在8.5至2.5 Gy之间的局部治疗指导原则。前提是细胞周期进程和增殖可忽略不计,此比例关系才有效。假设急性和晚期组织反应的特征是α/β值约为10和3 Gy,且单指数修复半衰期约为3小时,那么两种方法给予相同的总剂量大致等效。急性和晚期非造血正常组织损伤的等效剂量为:0.02 Gy/min和每次分次8.5 Gy;0.01 Gy/min和每次分次5.5 Gy;以及0.005 Gy/min和每次分次2.5 Gy。因此,要模拟分次剂量约为2 Gy的高剂量率放疗,需要非常低的剂量率,低于0.005 Gy/min。然而,比例因子取决于组织的修复半衰期。对已发表的关于正常组织反应剂量率效应的数据回顾表明,在低于0.02 Gy/min时,晚期效应的剂量率依赖性明显强于急性效应。各种急性非造血效应之间或各种晚期效应之间的剂量率依赖性没有显著差异。一致的剂量率依赖性证明了在分次剂量和剂量率之间使用通用比例因子是合理的,这与为各种正常组织效应计算的修复半衰期的广泛值形成对比。这表明目前用于修复动力学的模型并不令人满意。在低于0.02 Gy/min的临床剂量率范围内,实验数据也很少。因此,有必要进一步验证所提出的分次剂量和剂量率之间的比例关系。

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