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A mathematical model of the colon crypt capturing compositional dynamic interactions between cell types

机译:结肠隐窝捕获细胞类型之间组成动态相互作用的数学模型

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摘要

Models of the development and early progression of colorectal cancer are based upon understanding the cycle of stem cell turnover, proliferation, differentiation and death. Existing crypt compartmental models feature a linear pathway of cell types, with little regulatory mechanism. Previous work has shown that there are perturbations in the enteroendocrine cell population of macroscopically normal crypts, a compartment not included in existing models. We show that existing models do not adequately recapitulate the dynamics of cell fate pathways in the crypt. We report the progressive development, iterative testing and fitting of a developed compartmental model with additional cell types, and which includes feedback mechanisms and cross-regulatory mechanisms between cell types. The fitting of the model to existing data sets suggests a need to invoke cross-talk between cell types as a feature of colon crypt cycle models.
机译:大肠癌的发展和早期进展的模型是基于对干细胞更新,增殖,分化和死亡的周期的了解。现有的隐窝区室模型具有细胞类型的线性途径,几乎没有调节机制。先前的工作表明,宏观正常隐窝的肠内分泌细胞群存在扰动,该隐腔是现有模型中未包括的。我们表明,现有模型不能充分概括隐窝中细胞命运途径的动力学。我们报告了渐进的发展,迭代测试和开发的隔间模型与其他细胞类型的拟合,其中包括反馈机制和细胞类型之间的交叉调控机制。将模型与现有数据集进行拟合表明,有必要调用单元格类型之间的串扰,作为结肠隐窝周期模型的功能。

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