A computational study of VEGF production by patterned retinal epithelial cell colonies as a model for neovascular macular degeneration
Authored by Gregory J Podgorski, Nicholas S Flann, Qanita Bani Baker, Elizabeth Vargis
Date Published: 2017
DOI: 10.1186/s13036-017-0063-6
Sponsors:
United States National Institutes of Health (NIH)
Platforms:
No platforms listed
Model Documentation:
Other Narrative
Model Code URLs:
Model code not found
Abstract
Background: The configuration of necrotic areas within the retinal
pigmented epithelium is an important element in the progression of
age-related macular degeneration (AMD). In the exudative (wet) and
non-exudative (dry) forms of the disease, retinal pigment epithelial
(RPE) cells respond to adjacent atrophied regions by secreting vascular
endothelial growth factor (VEGF) that in turn recruits new blood vessels
which lead to a further reduction in retinal function and vision. In
vitro models exist for studying VEGF expression in wet AMD (Vargis et
al., Biomaterials 35(13): 3999-4004, 2014), but are limited in the
patterns of necrotic and intact RPE epithelium they can produce and in
their ability to finely resolve VEGF expression dynamics.
Results: In this work, an in silico hybrid agent-based model was
developed and validated using the results of this cell culture model of
VEGF expression in AMD. The computational model was used to extend the
cell culture investigation to explore the dynamics of VEGF expression in
different sized patches of RPE cells and the role of negative feedback
in VEGF expression. Results of the simulation and the cell culture
studies were in excellent qualitative agreement, and close quantitative
agreement.
Conclusions: The model indicated that the configuration of necrotic and
RPE cell-containing regions have a major impact on VEGF expression
dynamics and made precise predictions of VEGF expression dynamics by
groups of RPE cells of various sizes and configurations. Coupled with
biological studies, this model may give insights into key molecular
mechanisms of AMD progression and open routes to more effective
treatments.
Tags
Mechanisms
micropatterning
Expression
Size
Auto-regulation
Vascular endothelial growth factor
Age-related macular degeneration
Retinal pigment epithelial cells
Micropatterned surfaces
Secretion