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首页> 外文期刊>British Journal of Radiology >Cytogenetic assessment of heterogeneous radiation doses in cancer patients treated with fractionated radiotherapy.
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Cytogenetic assessment of heterogeneous radiation doses in cancer patients treated with fractionated radiotherapy.

机译:分次放疗治疗的癌症患者异种放射剂量的细胞遗传学评估。

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The purpose of this study was to evaluate the in vivo dose-response relation of chromosome aberration formation and distribution in a context of localised and fractionated radiotherapy. Cytogenetic analysis was applied to eight patients, all treated for the same tumour localisation; the same localisation was used to prevent the variability usually observed between patients treated with radiotherapy and to allow the corresponding roles of the size of irradiation field and of the dose rate to be studied. The yield of dicentrics, centric rings and fragments was measured in blood samples taken before treatment, during the course of radiotherapy and up to 6 months after. After the first fraction of radiotherapy, we observed that the whole-body dose estimated from the yield of dicentrics and rings was higher (0.35+/-0.2 Gy) than the calculated equivalent whole-body dose (0.07+/-0.04 Gy). By contrast, the partial-body dose derived from the Qdr (quotient of dicentrics and rings) model was estimated to be 2.2+/-0.3 Gy, which agreed quite well with the dose delivered to the tumour (2.1+/-0.1 Gy). We also found a correlation between the yield of induced chromosome aberrations and the target field size (p = 0.014). U-value analysis showed that the distribution of dicentrics and rings was overdispersed, despite the fractionation of the exposure, and a positive correlation between the U-value and the dose rate was observed (p = 0.017). Overall, these results suggest that the proportion of undamaged lymphocytes could increase with the dose rate.
机译:这项研究的目的是评估局部和分级放疗的情况下染色体畸变形成和分布的体内剂量反应关系。细胞遗传学分析应用于八名患者,所有患者均接受相同的肿瘤定位;使用相同的定位来防止通常在接受放射治疗的患者之间观察到差异,并允许研究辐射场大小和剂量率的相应作用。在治疗前,放疗过程中以及直至6个月后的血样中测量双着丝粒,中心环和碎片的产量。在放疗的第一部分后,我们观察到根据双着丝粒和环的产量估算的全身剂量(0.35 +/- 0.2 Gy)高于计算的当量全身剂量(0.07 +/- 0.04 Gy)。相比之下,从Qdr(双着丝粒和环的商)模型得出的局部剂量估计为2.2 +/- 0.3 Gy,这与传递给肿瘤的剂量非常吻合(2.1 +/- 0.1 Gy) 。我们还发现诱导染色体畸变的产量与目标视野大小之间存在相关性(p = 0.014)。 U值分析显示,尽管暴露程度有所不同,但双着丝粒和环的分布却过于分散,并且观察到U值与剂量率之间存在正相关关系(p = 0.017)。总体而言,这些结果表明未损伤淋巴细胞的比例可能随剂量率的增加而增加。

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