数值模拟评估不同结直肠癌细胞系在顺铂治疗中的行为

D. Šeklić, T. Djukić, M. Zivanovic, M. Jovanović, N. Filipovic
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引用次数: 0

摘要

结直肠癌是最常见的癌症类型之一,其转移是抗癌治疗中的一个特殊问题。因此,了解转移形成的关键步骤,如粘附连接的丢失是至关重要的。$\mathbf{E}$ -cadherin和$\beta$ -catenin是癌细胞中参与细胞-细胞连接的蛋白。本研究旨在通过数值模拟解释两种结直肠癌细胞系在标准抗癌药物顺铂治疗后E-cadherin和$\ β $ -catenin的变化。通过免疫荧光法测定E-cadherin和$\beta$ -catenin蛋白的表达,验证了数学模型的有效性。我们的研究结果表明,Wnt通路的数值模型完全证实了HCT-116细胞的实验结果,而对于SW-480细胞,该模型需要进行调整。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Numerical modelling in assessment of different colorectal cancer cell lines behavior in treatment with cisplatin
Colorectal cancer is one of the most common types of cancer and metastasis particular problem in anticancer treatment. Therefore, it is crucial to understand key steps in metastasis formation, such as loss of adherent junctions. $\mathbf{E}$ -cadherin and $\beta$ -catenin are proteins involved in cell-cell junctions in cancer cells. Present study aimed to explain changes in E-cadherin and $\beta$ -catenin in two colorectal cancer cell lines after treatment with standard anticancer drug cisplatin, by using numerical modelling. The validity of the mathematical model was tested by experimental measurement of E-cadherin and $\beta$ -catenin protein expression by immunofluorescent method. Our results shows that the numerical model of the Wnt pathway completely confirms experimental results for HCT-116 cells, while for SW-480 cells this model should be adjusted.
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