首页> 外文期刊>British Journal of Radiology >A four-dimensional computer simulation model of the in vivo response to radiotherapy of glioblastoma multiforme: studies on the effect of clonogenic cell density.
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A four-dimensional computer simulation model of the in vivo response to radiotherapy of glioblastoma multiforme: studies on the effect of clonogenic cell density.

机译:多形性胶质母细胞瘤对放疗的体内反应的三维计算机仿真模型:克隆细胞密度的影响研究。

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摘要

Tumours behave as complex, self-organizing, opportunistic dynamic systems. In an attempt to better understand and describe the highly complicated tumour behaviour, a novel four-dimensional simulation model of in vivo tumour growth and response to radiotherapy has been developed. This paper presents the latest improvements to the model as well as a parametric validation of it. Improvements include an advanced algorithm leading to conformal tumour shrinkage, a quantitative consideration of the influence of oxygenation on radiosensitivity and a more realistic, imaging based description of the neovasculature distribution. The tumours selected for the validation of the model are a wild type and a mutated p53 gene glioblastomas multiforme. According to the model predictions, a whole tumour with larger cell cycle duration tends to repopulate more slowly. A lower oxygen enhancement ratio value leads to a more radiosensitive whole tumour. Higher clonogenic cell density (CCD) produces a higher number of proliferating tumour cells and, therefore, a more difficult tumour to treat. Simulation predictions agree at least semi-quantitatively with clinical experience, and particularly with the outcome of the Radiation Therapy Oncology Group (RTOG) Study 83-02. It is stressed that the model allows a quantitative study of the interrelationship between the competing influences in a complex, dynamic tumour environment. Therefore, the model can already be useful as an educational tool with which to study, understand and demonstrate the role of various parameters in tumour growth and response to irradiation. A long term quantitative clinical adaptation and validation of the model aiming at its integration into the treatment planning procedure is in progress.
机译:肿瘤表现为复杂的,自组织的,机会主义的动态系统。为了更好地理解和描述高度复杂的肿瘤行为,已经开发了体内肿瘤生长和对放射疗法的反应的新型四维模拟模型。本文介绍了该模型的最新改进以及对其的参数验证。改进措施包括导致共形肿瘤缩小的先进算法,氧合作用对放射敏感性影响的定量考虑以及对新脉管系统分布的基于影像的更现实描述。选择用于验证模型的肿瘤是野生型和突变的多态性p53基因胶质母细胞瘤。根据模型预测,具有较大细胞周期持续时间的整个肿瘤趋向于更慢地繁殖。较低的氧增强比值导致对放射线敏感的整个肿瘤。较高的克隆细胞密度(CCD)会产生大量的增殖肿瘤细胞,因此,治疗起来更困难。模拟预测至少在定量上与临床经验相符,特别是与放射治疗肿瘤学组(RTOG)研究83-02的结果相符。需要强调的是,该模型允许对复杂,动态肿瘤环境中竞争影响之间的相互关系进行定量研究。因此,该模型已经可以用作研究,理解和证明各种参数在肿瘤生长和对辐射反应中的作用的教育工具。旨在对该模型整合到治疗计划程序中的模型的长期定量临床适应和验证正在进行中。

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