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Computational Model of Population Dynamics Based on the Cell Cycle and Local Interactions

机译:基于细胞周期和局部交互的人口动力学计算模型

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Our study bridges cellular (mesoscopic) level interactions and global population (macroscopic) dynamics of carcinoma. The morphological differences and transitions between well and smooth defined benign tumors and tentacular malignat tumors suggest a theoretical analysis of tumor invasion based on the development of mathematical models exhibiting bifurcations of spatial patterns in the density of tumor cells. Our computational model views the most representative and clinically relevant features of oncogenesis as a fight between two distinct sub-systems: the immune system of the host and the neoplastic system. We implemented the neoplastic sub-system using a three-stage cell cycle: active, dormant, and necrosis. The second considered sub-system consists of cytotoxic active (effector) cells — EC, with a very broad phenotype ranging from NK cells to CTL cells, macrophages, etc. Based on extensive numerical simulations, we correlated the fractal dimensions for carcinoma, which could be obtained from tumor imaging, with the malignat stage. Our computational model was able to also simulate the effects of surgical, chemotherapeutical, and radiotherapeutical treatments.
机译:我们的研究桥梁细胞(介观)水平相互作用和癌的全球人口(宏观)动态。良好和平滑定义的良性肿瘤与良性肿瘤之间的形态学差异和过渡表明了肿瘤侵袭的理论分析,基于肿瘤细胞密度的空间模式分叉的数学模型的发展。我们的计算模型观看了一种诱导性和临床相关特征,作为两个不同的子系统之间的斗争:宿主和肿瘤系统的免疫系统。我们使用三阶段细胞周期实施了肿瘤子系统:活性,休眠和坏死。第二次考虑的子系统由细胞毒性活性(效应)细胞 - EC组成,具有从NK细胞到CTL细胞,巨噬细胞等的非常宽的表型基于广泛的数值模拟,我们将癌的分形尺寸相关联,可以从肿瘤成像获得,利用Malignat阶段。我们的计算模型还能够模拟外科,化学治疗和放射治疗的影响。

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