An agent-based model for drug-radiation interactions in the tumour microenvironment: Hypoxia-activated prodrug SN30000 in multicellular tumour spheroids
Authored by Xinjian Mao, Sarah McManaway, Jagdish K Jaiswal, Priyanka B Patel, William R Wilson, Kevin O Hicks, Gib Bogle
Date Published: 2018
DOI: 10.1371/journal.pcbi.1006469
Sponsors:
Marsden Fund New Zealand
Platforms:
No platforms listed
Model Documentation:
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Model Code URLs:
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Abstract
Multicellular tumour spheroids capture many characteristics of human
tumour microenvironments, including hypoxia, and represent an
experimentally tractable in vitro model for studying interactions
between radiotherapy and anticancer drugs. However, interpreting
spheroid data is challenging because of limited ability to observe cell
fate within spheroids dynamically. To overcome this limitation, we have
developed a hybrid continuum/agent-based model (ABM) for HCT116 tumour
spheroids, parameterised using experimental models (monolayers and
multilayers) in which reaction and diffusion can be measured directly.
In the ABM, cell fate is simulated as a function of local oxygen,
glucose and drug concentrations, determined by solving diffusion
equations and intracellular reactions. The model is lattice-based, with
cells occupying discrete locations on a 3D grid embedded within a
coarser grid that encompasses the culture medium; separate solvers are
employed for each grid. The generated concentration fields account for
depletion in the medium and specify concentration-time profiles within
the spheroid. Cell growth and survival are determined by intracellular
oxygen and glucose concentrations, the latter based on direct
measurement of glucose diffusion/reaction (in multilayers) for the first
time. The ABM reproduces known features of spheroids including overall
growth rate, its oxygen and glucose dependence, peripheral cell
proliferation, central hypoxia and necrosis. We extended the ABM to
describe in detail the hypoxia-dependent interaction between ionising
radiation and a hypoxia-activated prodrug (SN30000), again using
experimentally determined parameters; the model accurately simulated
clonogenic cell killing in spheroids, while inclusion of reversible cell
cycle delay was required to account for the marked spheroid growth delay
after combined radiation and SN30000. This ABM of spheroid growth and
response exemplifies the utility of integrating computational and
experimental tools for investigating radiation/drug interactions, and
highlights the critical importance of understanding oxygen, glucose and
drug concentration gradients in interpreting activity of therapeutic
agents in spheroid models.
Tags
Simulation
cancer
systems
growth
Cell
Tissue
Solid tumor
Oxygen-transport
Cytotoxicity
Tirapazamine