3D hybrid modelling of vascular network formation
Authored by Barry D Hughes, Philip K Maini, Helen M Byrne, Holger Perfahl, Tomas Alarcon, Mark C Lloyd, Matthias Reuss
Date Published: 2017
DOI: 10.1016/j.jtbi.2016.11.013
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Abstract
We develop an off-lattice, agent-based model to describe vasculogenesis,
the de novo formation of blood vessels from endothelial progenitor cells
during development. The endothelial cells that comprise our vessel
network are viewed as linearly elastic spheres that move in response to
the forces they experience. We distinguish two types of endothelial
cells: vessel elements are contained within the network and tip cells
are located at the ends of vessels. Tip cells move in response to
mechanical forces caused by interactions with neighbouring vessel
elements and the local tissue environment, chemotactic forces and a
persistence force which accounts for their tendency to continue moving
in the same direction. Vessel elements are subject to similar mechanical
forces but are insensitive to chemotaxis. An angular persistence force
representing interactions with the local tissue is introduced to
stabilise buckling instabilities caused by cell proliferation. Only
vessel elements proliferate, at rates which depend on their degree of
stretch: elongated elements have increased rates of proliferation, and
compressed elements have reduced rates. Following division, the fate of
the new cell depends on the local mechanical environment: the
probability of forming a new sprout is increased if the parent vessel is
highly compressed and the probability of being incorporated into the
parent vessel increased if the parent is stretched. Simulation results
reveal that our hybrid model can reproduce the key qualitative
features-of vasculogenesis. Extensive parameter sensitivity analyses
show that significant changes in network size and morphology are induced
by varying the chemotactic sensitivity of tip cells, and the
sensitivities of the proliferation rate and the sprouting probability to
mechanical stretch. Varying the chemotactic sensitivity directly
influences the directionality of the networks. The degree of branching,
and thereby the density of the networks, is influenced by the sprouting
probability. Glyphs that simultaneously depict several network
properties are introduced to show how these and other network quantities
change over time and also as model parameters vary. We also show how
equivalent glyphs constructed from in vivo data could be used to
discriminate between normal and tumour vasculature and, in the longer
term, for model validation. We conclude that our biomechanical hybrid
model can generate vascular networks that are qualitatively similar to
those generated from in vitro and in vivo experiments.
Tags
Agent-based modelling
Angiogenesis
cancer
architecture
growth
Mechanisms
morphogenesis
In-vitro
Tumor-induced angiogenesis
Mathematical-models
Cell-migration
Vasculogenesis
Mechanical model
Normalization