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Thermodynamically constrained averaging theory for cancer growth modelling

机译:癌症生长建模的热力学限制平均理论

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In Systems Biology, network models are often used to describe intracellular mechanisms at the cellular level. The obtained results are difficult to translate into three dimensional biological systems of higher order. The multiplicity and time dependency of cellular system boundaries, mechanical phenomena and spatial concentration gradients affect the intercellular relations and communication of biochemical networks. These environmental effects can be integrated with our promising cancer modelling environment, that is based on thermodynamically constrained averaging theory (TCAT). Especially, the TCAT parameter viscosity can be used as critical player in tumour evolution. Strong cell-cell contacts and a high degree of differentiation make cancer cells viscous and support compact tumour growth with high tumour cell density and accompanied displacement of the extracellular material. In contrast, dedifferentiation and losing of cell-cell contacts make cancer cells more fluid and lead to an infiltrating tumour growth behaviour without resistance due to the ECM. The fast expanding tumour front of the invasive type consumes oxygen and the limited oxygen availability behind the invasive front results automatically in a much smaller average tumour cell density in the tumour core. The proposed modelling technique is most suitable for tumour growth phenomena in stiff tissues like skin or bone with high content of extracellular matrix.
机译:在系统生物学中,网络模型通常用于描述细胞水平的细胞内机制。所得结果难以转化为高阶的三维生物学系统。蜂窝系统边界,机械现象和空间浓度梯度的多重和时间依赖性影响生物化学网络的细胞间关系和通信。这些环境效应可以与我们有前途的癌症建模环境集成,这是基于热力学限制的平均理论(TCAT)。特别是,TCAT参数粘度可以用作肿瘤进化中的关键效果。强细胞 - 细胞触点和高度分化使癌细胞粘稠并支持具有高肿瘤细胞密度和细胞外材料的伴随的肿瘤生长。相反,微细胞化和丢失细胞细胞接触使癌细胞更流体,并导致渗透肿瘤生长行为而不会由于ECM而导致的抗性。侵入式肿瘤的快速膨胀肿瘤前部消耗氧气,并在肿瘤核心的平均平均肿瘤细胞密度下自动消耗氧气并在侵入前的前面结果后面的有限氧可用性。所提出的建模技术最适合肿瘤生长现象,如皮肤或骨骼的僵硬组织,具有高含量的细胞外基质。

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