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首页> 外文期刊>British Journal of Radiology >The potential for mathematical modelling in the assessment of the radiation dose equivalent of cytotoxic chemotherapy given concomitantly with radiotherapy.
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The potential for mathematical modelling in the assessment of the radiation dose equivalent of cytotoxic chemotherapy given concomitantly with radiotherapy.

机译:数学模型在评估放疗同时给予的细胞毒性化学疗法的放射剂量当量方面的潜力。

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The linear quadratic (LQ) concept of biological effective dose (BED) is used with Poisson statistics to estimate the radiation equivalent BED of cytotoxic chemotherapy (CBED) that would provide improvements in tumour control probability (TCP) typically achieved in randomized clinical trials of chemoradiation. The concepts of pure radio-sensitization and independent chemotherapy cell kill are represented by mathematical equations. Small values of sensitizer enhancement ratios (s) can provide modest increases in TCP when large numbers of radiotherapy fractions are sensitized; larger s values are required if only a small number of radiotherapy fractions are sensitized. Independent chemotherapy induced cell kill is sufficient to explain the benefits achieved with concomitant chemoradiotherapy in situations where a sufficiently high chemotherapy dose intensity is used (i.e. the dose-time intensity of cytotoxic chemotherapy without radiation is considered to be sufficient to cause significant tumour regression although not cure). Care is required in the use of the Poisson cure probability model because of the associated steep dose-response curves that may underestimate both s and the CBED. By use of random sampling methods and estimation over a theoretical population of different tumours, more robust results are obtained with dose-response curves that correspond better to those in clinical data sets. These predict a 2-4 Gy(10) equivalent for each pulse of chemotherapy such as single agent Cis-Platinum when used weekly during radiotherapy for a maximum of 4 cycles. This preliminary paper does not consider normal tissue complication probabilities, of which there are relatively few mature results for modern chemoradiotherapy. The BED concept can be used to estimate the equivalent dose of radiotherapy that will achieve the same cell kill as concomitant cytotoxic chemotherapy. Relatively simple radiobiological modelling can be used to guide decision-making regarding the assessment of the most appropriate combined modality schedules, and has important implications in the design of clinical trials.
机译:生物有效剂量(BED)的线性二次(LQ)概念与Poisson统计一起使用,以估算细胞毒性化学疗法(CBED)的辐射当量BED,这将改善通常在化学放疗的随机临床试验中实现的肿瘤控制概率(TCP) 。纯粹的放射增敏和独立的化学杀伤细胞的概念由数学方程式表示。当对大量放射治疗部位进行敏化时,较小的敏化剂增强比值可以使TCP适度增加;如果仅对少量放射治疗部分进行敏化,则需要更大的s值。在使用足够高的化疗剂量强度的情况下,独立的化学疗法诱导的细胞杀伤足以解释伴随放化疗所带来的益处(即,没有辐射的细胞毒性化学疗法的剂量-时间强度足以引起显着的肿瘤消退,尽管并非如此)治愈)。由于可能会低估s和CBED的相关陡峭剂量反应曲线,因此在使用Poisson治愈概率模型时需要格外小心。通过使用随机抽样方法并在不同肿瘤的理论人群中进行估计,可以获得剂量/剂量曲线更稳健的结果,这些剂量-剂量曲线与临床数据更好地对应。这些预测在放疗期间每周使用最多4个周期时,每个化学疗法脉冲(例如单药顺铂)的等效脉冲为2-4 Gy(10)。该初步论文未考虑正常组织并发症的可能性,而现代化学放疗的成熟结果相对较少。 BED概念可用于估计与伴随细胞毒性化学疗法可达到相同细胞杀伤率的放射疗法的等效剂量。相对简单的放射生物学建模可用于指导有关最合适的联合治疗方案时间表评估的决策,并且在临床试验设计中具有重要意义。

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