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动态多叶准直器调强放射治疗剂量输送后细胞存活的体外研究。

In vitro study of cell survival following dynamic MLC intensity-modulated radiation therapy dose delivery.

作者信息

Moiseenko Vitali, Duzenli Cheryl, Durand Ralph E

机构信息

Vancouver Cancer Centre, British Columbia Cancer Agency, 600 West 10th Avenue, Vancouver, British Columbia V5Z 4E6, Canada.

出版信息

Med Phys. 2007 Apr;34(4):1514-20. doi: 10.1118/1.2712044.

Abstract

The possibility of reduced cell kill following intensity-modulated radiation therapy (IMRT) compared to conventional radiation therapy has been debated in the literature. This potential reduction in cell kill relates to prolonged treatment times typical of IMRT dose delivery and consequently increased repair of sublethal lesions. While there is some theoretical support to this reduction in cell kill published in the literature, direct experimental evidence specific to IMRT dose delivery patterns is lacking. In this study we present cell survival data for three cell lines: Chinese hamster V79 fibroblasts, human cervical carcinoma, SiHa and colon adenocarcinoma, WiDr. Cell survival was obtained for 2.1 Gy delivered as acute dose with parallel-opposed pair (POP), irradiation time 75 s, which served as a reference; regular seven-field IMRT, irradiation time 5 min; and IMRT with a break for multiple leaf collimator (MLC) re-initialization after three fields were delivered, irradiation time 10 min. An actual seven-field dynamic MLC IMRT plan for a head and neck patient was used. The IMRT plan was generated for a Varian EX or iX linear accelerator with 120 leaf Millenium MLC. Survival data were also collected for doses 1X, 2X, 3X, 4X, and 5x 2.1 Gy to establish parameters of the linear-quadratic equation describing survival following acute dose delivery. Cells were irradiated inside an acrylic cylindrical phantom specifically designed for this study. Doses from both IMRT and POP were validated using ion chamber measurements. A reproducible increase in cell survival was observed following IMRT dose delivery. This increase varied from small for V79, with a surviving fraction of 0.8326 following POP vs 0.8420 following uninterrupted IMRT, to very pronounced for SiHa, with a surviving fraction of 0.3903 following POP vs 0.5330 for uninterrupted IMRT. When compared to IMRT or IMRT with a break for MLC initialization, cell survival following acute dose delivery was significantly different, p < 0.05, in three out of six cases. In contrast, when cell survival following IMRT was compared to that following IMRT with a break for MLC initialization the difference was always statistically insignificant. When projected to a 30 fraction treatment, dose deficit to bring cell survival to the same value as in POP was calculated as 4.1, 24.9, and 31.1 Gy for V79, WiDr, and SiHa cell lines, respectively. The dose deficit did not relate to the alpha/beta ratio obtained in this study for the three cell lines. Clinical data do not show reduction in local control following IMRT. Possible reasons for this are discussed. The obtained data set can serve as a test data set for models designed to explore the effect of dose delivery prolongation/fractionation in IMRT on radiation therapy outcome.

摘要

与传统放射治疗相比,调强放射治疗(IMRT)后细胞杀伤减少的可能性在文献中一直存在争议。这种细胞杀伤的潜在减少与IMRT剂量递送典型的较长治疗时间有关,因此亚致死性损伤的修复增加。虽然文献中有一些关于这种细胞杀伤减少的理论支持,但缺乏针对IMRT剂量递送模式的直接实验证据。在本研究中,我们展示了三种细胞系的细胞存活数据:中国仓鼠V79成纤维细胞、人宫颈癌SiHa细胞系和结肠腺癌WiDr细胞系。以平行相对野(POP)方式给予2.1 Gy急性剂量,照射时间75秒,作为参考获得细胞存活率;常规七野IMRT,照射时间5分钟;以及在照射三野后进行多叶准直器(MLC)重新初始化中断的IMRT,照射时间10分钟。使用了一名头颈患者的实际七野动态MLC IMRT计划。IMRT计划是为配备120叶Millenium MLC的Varian EX或iX直线加速器生成的。还收集了1X、2X、3X、4X和5×2.1 Gy剂量的存活数据,以建立描述急性剂量递送后存活情况的线性二次方程参数。细胞在专门为此研究设计的丙烯酸圆柱形体模内进行照射。IMRT和POP的剂量均通过电离室测量进行验证。在IMRT剂量递送后观察到细胞存活率有可重复的增加。这种增加程度因细胞系而异,对于V79细胞系较小,POP照射后的存活分数为0.8326,不间断IMRT照射后的存活分数为0.8420;对于SiHa细胞系则非常明显,POP照射后的存活分数为0.3903,不间断IMRT照射后的存活分数为0.5330。与IMRT或MLC初始化中断的IMRT相比,急性剂量递送后的细胞存活率在六分之三的情况下有显著差异,p<0.05。相比之下,当将IMRT后的细胞存活率与MLC初始化中断的IMRT后的细胞存活率进行比较时,差异始终无统计学意义。当推算至30次分割治疗时,将V79、WiDr和SiHa细胞系的细胞存活率提高到与POP相同水平所需的剂量不足分别计算为4.1、24.9和31.1 Gy。剂量不足与本研究中三种细胞系获得的α/β比值无关。临床数据未显示IMRT后局部控制率降低。讨论了可能的原因。所获得的数据集可作为测试数据集,用于旨在探索IMRT中剂量递送延长/分割对放射治疗结果影响的模型。

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