Agent-based model illustrates the role of the microenvironment in regeneration in healthy and mdx skeletal muscle
Authored by Silvia S Blemker, Kelley M Virgilio, Kyle S Martin, Shayn M Peirce
Date Published: 2018
DOI: 10.1152/japplphysiol.00379.2018
Sponsors:
United States National Institutes of Health (NIH)
United States National Science Foundation (NSF)
Platforms:
No platforms listed
Model Documentation:
Other Narrative
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Model Code URLs:
Model code not found
Abstract
Duchenne muscular dystrophy (DMD) is a progressive muscle-wasting
disease with no effective treatment. Multiple mechanisms are thought to
contribute to muscle wasting, including increased susceptibility to
contraction-induced damage, chronic inflammation, fibrosis, altered
satellite stem cell (SSC) dynamics, and impaired regenerative capacity.
The goals of this project were to 1) develop an agent-based model of
skeletal muscle that predicts the dynamic regenerative response of
muscle cells, fibroblasts, SSCs, and inflammatory cells as a result of
contraction-induced injury, 2) calibrate and validate the model
parameters based on comparisons with published experimental
measurements, and 3) use the model to investigate how changing isolated
and combined factors known to be associated with DMD (e.g., altered
fibroblast or SSC behaviors) influence muscle regeneration. Our
predictions revealed that the percent of injured muscle that recovered
28 days after injury was dependent on the peak SSC counts following
injury. In simulations with near-full crosssectional area recovery
(healthy, 4-wk mdx, 3-mo mdx), the SSC counts correlated with the extent
of initial injury; however, in simulations with impaired regeneration
(9-mo mdx), the peak SSC counts were suppressed relative to initial
injury. The differences in SSC counts between these groups were emergent
predictions dependent on altered microenvironment factors known to be
associated with DMD. Multiple cell types influenced the peak number of
SSCs, but no individual parameter predicted the differences in SSC
counts. This finding suggests that interventions to target the
microenvironment rather than SSCs directly could be an effective method
for improving regeneration in impaired muscle.
NEW \& NOTEWORTHY A computational model predicted that satellite stem
cell (SSC) counts are correlated with muscle crosssectional area (CSA)
recovery following injury. In simulations with impaired CSA recovery,
SSC counts are suppressed relative to healthy muscle. The suppressed SSC
counts were an emergent model prediction, because all simulations had
equal initial SSC counts. Fibroblast and anti-inflammatory macrophage
counts influenced SSC counts, but no single factor was able to predict
the pathological differences in SSC counts that lead to impaired
regeneration.
Tags
Agent-based model
Stem-cells
Self-renewal
Mouse model
Growth-factor-i
Satellite cells
Duchenne muscular dystrophy
Skeletal muscle
Duchenne muscular-dystrophy
Tibialis anterior muscles
Fibro/adipogenic progenitors
Fibroblast
migration
Soleus muscles