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首页> 外文期刊>International Journal of Radiation Biology: Covering the Physical, Chemical, Biological, and Medical Effects of Ionizing and Non-ionizing Radiations >Flow cytometry-assisted Monte Carlo simulation predicts clonogenic survival of cell populations with lognormal distributions of radiopharmaceuticals and anticancer drugs
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Flow cytometry-assisted Monte Carlo simulation predicts clonogenic survival of cell populations with lognormal distributions of radiopharmaceuticals and anticancer drugs

机译:流式细胞术辅助的蒙特卡洛模拟预测放射性药物和抗癌药物的对数正态分布的细胞群体的克隆形成存活

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摘要

Purpose: Although the distribution of therapeutic agents within cell populations may appear uniform at the macroscopic level, the distribution at the multicellular level is nonuniform. As such, the mean agent concentration in tissue may not be a suitable quantity for use in predicting biological effects. Failure in chemotherapy and targeted radionuclide therapy has been attributed, in part, to the ubiquity of lognormal distributions of therapeutic agents. To improve capacity to predict biological response, this work develops approaches that determine the fate of a cell population on a cell-by-cell basis. Methods: Incorporation of the α-particle emitting radiochemical ( 210Po-citrate) and two anticancer drugs (daunomycin and doxorubicin) by Chinese hamster V79 cells was determined using flow cytometry. Monte Carlo simulation was used to estimate cell survival on the bases of mean and individual cell incorporation of each cytotoxic agent. The interrelationships between the Monte Carlo simulated cell survival and clonogenic cell survival were evaluated. Results: Cell survival obtained by Monte Carlo simulation based on individual cell incorporation was in good agreement with clonogenic cell survival for all agents. However, the agreement was poor when the simulation was carried out using the mean cell incorporation of the agents. Conclusion: These data indicate that, with the aid of flow cytometry, Monte Carlo simulations can be used to predict the toxicity of therapeutic agents in a manner that takes into account the effects of lognormal and other nonuniform distributions of agents within cell populations.
机译:目的:尽管治疗药物在细胞群体中的分布在宏观水平上可能看起来是均匀的,但在多细胞水平上的分布却是不均匀的。因此,组织中的平均药剂浓度可能不是用于预测生物学效应的合适量。化疗和靶向放射性核素治疗的失败部分归因于治疗剂的对数正态分布。为了提高预测生物学反应的能力,这项工作开发了确定每个细胞的细胞群命运的方法。方法:利用流式细胞仪测定了中国仓鼠V79细胞中α发射放射化学物质(210Po-柠檬酸盐)和两种抗癌药物(道诺霉素和阿霉素)的掺入情况。蒙特卡罗模拟用于基于每种细胞毒性剂的均值和单个细胞掺入来估计细胞存活。评估了蒙特卡洛模拟细胞存活率与克隆细胞存活率之间的相互关系。结果:通过蒙特卡罗模拟获得的基于单个细胞掺入的细胞存活率与所有药物的克隆细胞存活率非常一致。然而,当使用试剂的平均细胞掺入进行模拟时,一致性差。结论:这些数据表明,借助于流式细胞仪,蒙特卡洛模拟可用于考虑细胞对数正态分布和其他不均匀分布的影响,从而预测治疗剂的毒性。

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