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首页> 外文期刊>Radiotherapy and oncology: Journal of the European Society for Therapeutic Radiology and Oncology >Pre-treatment number of clonogenic cells and their radiosensitivity are major determinants of local tumour control after fractionated irradiation.
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Pre-treatment number of clonogenic cells and their radiosensitivity are major determinants of local tumour control after fractionated irradiation.

机译:克隆形成细胞的预处理数量及其放射敏感性是分次照射后局部肿瘤控制的主要决定因素。

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OBJECTIVE: The response of tumours to fractionated radiotherapy is determined by many factors including repopulation, reoxygenation, the number of clonogenic cells, and their intrinsic radiosensitivity. However, after single radiation doses given under conditions of clamp hypoxia, the dose to control a tumour locally is dependent only on the number of clonogenic cells and their cellular radiosensitivity. Therefore, these parameters were investigated using local control after single doses given under hypoxia, to predict the outcome of fractionated irradiation. MATERIALS AND METHODS: Ten hSCC cell lines (FaDu, UT-SCC-15, UT-SCC-14, XF354, UT-SCC-5, UT-SCC-45, SAS, CAL-33, UT-SCC-8, and HSC-4) were transplanted subcutaneously into the right hind-leg of NMRI nude mice. At 7mm in diameter, tumours were irradiated either with graded single doses under clamp blood flow conditions (n=873) or with 30 graded fractions within 6 weeks (n=905) under ambient conditions. Local tumour control was determined 120 days after irradiation. Radiation response was quantified in terms of TCD(50), i.e. the dose required to control 50% of tumours locally. RESULTS: Ten tumour lines investigated showed a pronounced heterogeneity in both TCD(50(30fx/6w)) after fractionated irradiation and TCD(50(SDclamp)) after single dose irradiation. TCD(50(30fx/6w)) varied between 45Gy for UT-SCC-45 and 127Gy for SAS; TCD(50(SDclamp)) varied between 42Gy for UT-SCC-14 and 66Gy for CAL-33. Two tumours were excluded from further analysis due to immunogenicity or non-defined TCD(50). Linear regression analysis revealed a significant positive correlation between TCD(50(SDclamp)) and TCD(50(30fx/6w)) (R(2)=0.82, p=0.002). CONCLUSIONS: Significant association between TCD(50(SDclamp)) and TCD(50(30fx/6w)) suggests that the pre-treatment number of clonogenic tumour cells and their cellular radiosensitivity have a major impact on local control after fractionated radiotherapy.
机译:目的:肿瘤对分级放疗的反应由许多因素决定,包括再填充,再充氧,克隆细胞的数量及其固有的放射敏感性。但是,在钳夹缺氧的条件下给予单次辐射剂量后,局部控制肿瘤的剂量仅取决于克隆细胞的数量及其细胞放射敏感性。因此,在缺氧条件下单次给药后,使用局部对照研究了这些参数,以预测分次照射的结果。材料与方法:十个hSCC细胞系(FaDu,UT-SCC-15,UT-SCC-14,XF354,UT-SCC-5,UT-SCC-45,SAS,CAL-33,UT-SCC-8和将HSC-4)皮下移植到NMRI裸鼠的右后腿。在直径为7mm的情况下,在钳夹血流条件下(n = 873)用分级单剂量照射肿瘤,或在环境条件下在6周内(n = 905)用30个分级分数照射肿瘤。照射120天后确定局部肿瘤对照。辐射反应以TCD(50)表示,即局部控制50%肿瘤所需的剂量。结果:十个肿瘤细胞系在分次照射后的TCD(50(30fx / 6w))和单剂量照射后的TCD(50(SDclamp))中均表现出明显的异质性。 TCD(50(30fx / 6w))在UT-SCC-45的45Gy和SAS的127Gy之间变化; TCD(50(SDclamp))在UT-SCC-14为42Gy和CAL-33为66Gy之间变化。由于免疫原性或不确定的TCD(50),两个肿瘤被排除在进一步分析之外。线性回归分析显示TCD(50(SDclamp))和TCD(50(30fx / 6w))之间存在显着正相关(R(2)= 0.82,p = 0.002)。结论:TCD(50(SDclamp))和TCD(50(30fx / 6w))之间的显着相关性表明,分次放疗后克隆形成的肿瘤细胞的预处理数量及其细胞放射敏感性对局部控制有重要影响。

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