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Modeling Growth of a Heterogeneous Tumor.

机译:模拟异质性肿瘤的生长。

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It has long been recognized that the growth of tumor population depends on the initial age distribution of the cells in the tumor and the age-dependent cellular birth rate. Deterministic dual-cell models have been available for sometime; these models take into account the effects of the resultant cell heterogeneity. Nevertheless, these models ignore various variables significantly affecting the growth, such as those characterizing the cells' inherent properties and environmental factors. Uncertainties, or fluctuations, arise when the growth is simulated with the models. Stochastic analysis of these fluctuations is the focus of the current work.Two types of cells are visualized to proliferate separately and to transform mutually during the process. The master equations of the system have been formulated through probabilistic population balance around a particular state by considering all mutually exclusive events. The governing equations for the means, variances, and covariance of the random variables have been derived through the system-size expansion of these nonlinear master equations. The stochastic pathways of the two different types of cells have been numerically simulated by the algorithm derived from the master equation for two different physical situations, one without and, the other, with the chemotherapeutic treatment. The results of the current study illuminate the significance of stochastically modeling the responses of the tumor to a variety of medicinal treatments: The coefficient of variation of the malignant cells' population magnifies with time under chemotherapeutic regimens. Consequently, the impact of the uncertainties in the exact number of malignant cells as expressed by this coefficient of variation is highly unpredictable. For example, it becomes increasingly uncertain if or how fast these cells will reactivate to become a full-blown carcinogenic tumor after treatment.
机译:早已认识到,肿瘤种群的增长取决于肿瘤细胞的初始年龄分布和年龄依赖性细胞的出生率。确定性双单元模型已经有一段时间了。这些模型考虑了所得细胞异质性的影响。然而,这些模型忽略了显着影响生长的各种变量,例如那些表征细胞固有特性和环境因素的变量。用模型模拟增长时会出现不确定性或波动。对这些波动的随机分析是当前工作的重点。在此过程中,两种类型的细胞可以分别增殖并相互转化。该系统的主要方程式是通过考虑所有相互排斥的事件,通过围绕特定状态的概率总体平衡来制定的。通过这些非线性主方程的系统大小展开,得出了随机变量的均值,方差和协方差的控制方程。两种不同类型的细胞的随机路径已通过从主方程导出的算法针对两种不同的物理情况进行了数值模拟,一种是不使用化学治疗,另一种是使用化学治疗。本研究的结果阐明了随机模拟肿瘤对多种药物治疗反应的重要性:在化疗方案下,恶性肿瘤细胞群的变异系数会随时间放大。因此,由该变化系数表示的恶性细胞确切数目的不确定性的影响是高度不可预测的。例如,治疗后这些细胞是否或以多快的速度重新活化成为成熟的致癌肿瘤变得越来越不确定。

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