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Agent Based Models of the Acute Inflammatory Response: Update on Development and Future Directions

Agent Based Models of the Acute Inflammatory Response: Update on Development and Future Directions. Swarmfest 2004, Ann Arbor, MI May 11, 2004 Gary An, MD Department of Trauma Cook County Hospital. Acute Inflammatory Response (AIR). Initial defense and repair mechanism

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Agent Based Models of the Acute Inflammatory Response: Update on Development and Future Directions

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  1. Agent Based Models of the Acute Inflammatory Response:Update on Development and Future Directions Swarmfest 2004, Ann Arbor, MI May 11, 2004 Gary An, MD Department of Trauma Cook County Hospital

  2. Acute Inflammatory Response (AIR) • Initial defense and repair mechanism • Specialized cellular/molecular pathways • Diffusely distributed/Tissue Nonspecific • Activation is non-specific to insult • Precedes Adaptive Immune response (self/non-self distinction=>Antibodies)

  3. Systemic Inflammatory Response Syndrome/Multiple Organ Failure (SIRS/MOF) • Disease of the ICU => “Unexplored State” • Pathologic state of Acute Immune Response (AIR) • Physiologic manifestations result from endogenous mediators • Hyperinflammation vs. Immune-suppression =>Temporal and Spatial

  4. Challenge of SIRS/MOF • Gap between Pathophysiology and Diagnosis • Gap between Mechanisms and Treatment • Gap between Basic Science and Clinical Implementation • Nonlinear Behavior => Complexity

  5. Components Rules Locality Emergent Properties Unexpected Behavior Cells Cellular Programming Membranes/ Receptors Organ Physiology SIRS/MOF AIR as a Complex System

  6. Applications of ABM to AIR/SIRS/MOF • Base Global Model • Pathophysiology • Therapeutic Interventions • Specific Disease Processes/Pathogens/Mechanism • Cutaneous and Inhalational Anthrax • Basic Science Experiment Simulation • Epithelial Permeability Model

  7. ABM of Global Systemic Inflammation • Endothelial/Blood interface • Activation/Propagation of Inflammation • Endothelial Cells and White Blood Cells • Dynamics of Pathophysiology • Proto-Testing Platform for Systemic Therapies • Very Abstract!

  8. Current Model of Global Inflammation

  9. Validation Strategies • Agent Rules=>Transparency wrt code • Behavior of Individual wrt global response to injury=>Individual Dynamics • Behavior of Population wrt cytokine patterns=>Population Dynamics • Behavior of Population wrt outcome to intervention=>Population Response

  10. Individual Response Dynamics • Four possible dynamics: • Successful healing • “Phase II” or Immune-suppressed SIRS/MOF • “Phase I” or Hyper-inflammatory SIRS/MOF • Overwhelming insult/infection • Function of degree of Initial Insult

  11. Population Dynamics:Cytokine Profiles • Patterns of cytokine levels for a population at a specific IIN • 7 days simulated time • IIN generates 50% mortality • N=100 • Pattern Oriented/Qualitative (Very Large Range-not shown)

  12. Population Response:Simulating Anti-inflammatory Interventions • Any mediator represented as a variable can be manipulated • Modified based on published effects • No other modifications of the ABM other than simulated intervention • Results all generated prospectively

  13. List of In-Silico Experiments

  14. ABM of Anthrax Infection • Modification of Base Global Model • Specific Characteristics of B. anthracis • Both Cutaneous and Inhalational Forms • Reproduce effects of Toxin-Component (Lethal Factor, Edema Factor and Protective Antigen) knockout species of B. anthracis

  15. Time of Death Distributions in All Modes

  16. Basic Science ABMs • Basic Science Paradigm = Linear analysis • Examine Component Sub-Systems • Improve efficiency of Basic Science experiments • Guide further investigation • Modular Components of System-wide Model

  17. ABM of Epithelial Cell Permeability: Structure • Based on model of Delude • Epithelial cell culture => Grid of Epi Cell Agents • Agent rules => Tight Junction (TJ) Formation • TJ status determines permeability

  18. ABM of Epithelial Cell Permeability: Results • Increased Permeability to NO/Pro-inflammatory cytokine mix • Blocked with NO scavenger/iNOS inhibitor • Matches Basic Science results • Potential Modular Model

  19. Uses of ABM of the AIR • Formalize Mental Models • Functional Repository of Basic Science Information • Modular • Community-dependent • Drug Engineering • Identify targets for manipulation • Use to pre-test a planned treatment regimes => Multi-Modal regimes

  20. Uses of ABM of the AIR cont. • Clinical Therapeutics Design • Patient Population Sub-stratification • Generate Cytokine Profiles => “Finer Grained” • Theoretical Tool • Mathematical characterization of system to guide future therapies • “Cross Platform” Validation

  21. Future Development • Multi-Tissue Model • Directional Flow • Coagulation • Multiple Organ Failure/Support • Modular Model • Basic Science Models • Community/Web-based • “Functional Data-bank”

  22. Complex Systems • Rules drive Local interactions between individual components • Feedback loops =>non-linearity • Interaction dynamics result in meta-stable structures=> Emergence • Hierarchies of Emergent properties • Non-intuitive, paradoxical behavior

  23. Agent Based Modeling (ABM) • System of Components=>Agents • Agent Rule systems=>Basic Science • Populations of agents in virtual world • Runs = agent actions/interactions=> Locality • Multiple runs=Random Number Generators=> basic science experiments • Stochastic and Deterministic

  24. Why use ABM to model AIR/SIRS/MOF? • Lots of information about potential agents (cells and molecules) • Process is driven by local interactions • Dynamics may be too complex for top-down modeling • Multiple possible levels of model validation • Integration of Models => Total System

  25. Doing Science with ABM • In-Silico Experiments => Virtual control and experimental populations • Apply standard statistical tools • Use Pattern Oriented Analysis • Formalize mental model building/testing hypotheses • Develop Theories

  26. Population Runs • Random number generators are active=> Heterogeneity • Multiple runs at a specific IIN generates a study “population” • Generates a “mortality rate” for a particular IIN (Mortality at >80% Total Damage)=>“Control Population”

  27. Results of In-Silico Experiments in Sterile Mode (n=100)

  28. Results of In-Silico Experiments in Infectious Mode (n=100)

  29. End Oxy Deficit Distributions in All Modes

  30. What ABM is not! • NOT a replacement of current techniques of scientific investigation. => “Software vs. Hardware” • NOT a clinical tool to provide a prognosis or determine a treatment course for an individual patient*

  31. Translation, Synthesis and ABMs • Requires data from Basic Science • “What we look for and find out.” • Places it into Synthetic framework • “How do the pieces fit together.” • Uses Multiple Hierarchies • “Little pieces make big pieces.” • We Do This Already! • Mental Models => Software Engineering

  32. “Theories of SIRS/MOF” • “Dynamic Equilibrium”=>Response is appropriate, degree is not • Concept of “anatomic containment” and “physiologic containment” • Identify “Amplifiers” of response • Importance of all aspects of the response => “If a mediator does a lot of different stuff don’t mess with it.” • Supplementation, not Blockade (WBCs smarter than ICU MDs)

  33. Summary of Key Points • The Acute Inflammatory Response is a complex system that cannot be fully characterized using existing techniques. • Agent Based Modeling is well suited to modeling the Inflammatory Response. • ABM would be an useful adjunct to existing techniques of investigation.

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