Autophagy capacity and sub-mitochondrial heterogeneity shape Bnip3-induced mitophagy regulation of apoptosis
Authored by Anne Hamacher-Brady, Sehyo Charley Choe, Nathan Ryan Brady
Date Published: 2015
DOI: 10.1186/s12964-015-0115-9
Sponsors:
German Federal Ministry of Education and Research (BMBF)
German Cancer Research Center (DKFZ)
Initiative and Networking Fund of the Helmholtz Association (NRB)
Platforms:
MATLAB
Model Documentation:
Other Narrative
Flow charts
Model Code URLs:
Model code not found
Abstract
Background: Mitochondria are key regulators of apoptosis. In response to
stress, BH3-only proteins activate pro-apoptotic Bcl2 family proteins
Bax and Bak, which induce mitochondrial outer membrane permeabilization
(MOMP). While the large-scale mitochondrial release of pro-apoptotic
proteins activates caspase-dependent cell death, a limited release
results in sub-lethal caspase activation which promotes tumorigenesis.
Mitochondrial autophagy (mitophagy) targets dysfunctional mitochondria
for degradation by lysosomes, and undergoes extensive crosstalk with
apoptosis signaling, but its influence on apoptosis remains
undetermined. The BH3-only protein Bnip3 integrates apoptosis and
mitophagy signaling at different signaling domains. Bnip3 inhibits
pro-survival Bcl2 members via its BH3 domain and activates mitophagy
through its LC3 Interacting Region (LIR), which is responsible for
binding to autophagosomes. Previously, we have shown that
Bnip3-activated mitophagy prior to apoptosis induction can reduce
mitochondrial activation of caspases, suggesting that a reduction to
mitochondrial levels may be pro-survival. An outstanding question is
whether organelle dynamics and/or recently discovered subcellular
variations of protein levels responsible for both MOMP sensitivity and
crosstalk between apoptosis and mitophagy can influence the cellular
apoptosis decision event. To that end, here we undertook a systems
biology analysis of mitophagy-apoptosis crosstalk at the level of
cellular mitochondrial populations.
Results: Based on experimental findings, we developed a multi-scale, hybrid model with an individually adaptive mitochondrial population, whose actions are determined by protein levels, embedded in an
agent-based model (ABM) for simulating subcellular dynamics and local
feedback via reactive oxygen species signaling. Our model, supported by
experimental evidence, identified an emergent regulatory structure
within canonical apoptosis signaling. We show that the extent of
mitophagy is determined by levels and spatial localization of autophagy
capacity, and subcellular mitochondrial protein heterogeneities. Our
model identifies mechanisms and conditions that alter the mitophagy
decision within mitochondrial subpopulations to an extent sufficient to
shape cellular outcome to apoptotic stimuli.
Conclusion: Overall, our modeling approach provides means to suggest new
experiments and implement findings at multiple scales in order to
understand how network topologies and subcellular heterogeneities can
influence signaling events at individual organelle level, and hence, determine the emergence of heterogeneity in cellular decisions due the
actions of the collective intra-cellular population.
Tags
Cytochrome-c release
Cell-death
E3 ligase
Membrane permeabilization
Mediated mitophagy
Cardiac myocytes
Dna-damage
Bcl-xl
Bnip3
Degradation