Modeling of stem cell dynamics in human colonic crypts in silico
Authored by Yuki Kagawa, Noriko Horita, Hideki Taniguchi, Satoshi Tsuneda
Date Published: 2014
DOI: 10.1007/s00535-013-0887-x
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Mathematical description
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Abstract
Several possible scenarios of cellular dynamics in human colonic crypts
have been inferred from transgenic animal experiments. However, because
of the discrepancy in size and physiology between humans and animals, quantitative predictions of tissue renewal and cancer development are
difficult to execute.
A two-dimensional individual based model was developed for the first
time to predict cellular dynamics in human colonic crypts. A simple
scenario, in which stem cells were not fixed positionally, divide
symmetrically and asymmetrically in a stochastic fashion in the lower
part of the crypt, was proposed and implemented in the developed model.
Numerical simulations of the model were executed in silico.
By comparing the results of computational simulations with available
experimental data, the presented scenario was consistent with various
experimental evidence. Using this scenario, we simulated and visualized
monoclonal conversion in the human colonic crypt. We also predicted that
the propensity for monoclonal expansion of a mutant cell was largely
dependent on the phenotype, the cell type, the position and the state of
the crypt.
Using the computational framework developed in this study, model users
can verify possible scenarios of stem cell dynamics occurring in human
colonic crypts and quantitatively predict cell behavior. Its
applicability in scenario verification and predictability makes it a
valuable tool for elucidation of stem cell dynamics in human colonic
crypts.
Tags
cancer
population
computational model
Tissue
Lgr5
Methylation patterns
Small-intestine
Immortal
model
Marker
Overpopulation