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Comparing ordinary and delay differential equations models for human gastric acid secretion

Comparing ordinary and delay differential equations models for human gastric acid secretion. Denise Kirschner, PhD Department of Microbiology and Immunology University of Michigan Medical School Ann Arbor, Michigan USA. Outline of lecture. Context of problem- H. pylori

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Comparing ordinary and delay differential equations models for human gastric acid secretion

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  1. Comparing ordinary and delay differential equations models for human gastric acid secretion Denise Kirschner, PhD Department of Microbiology and Immunology University of Michigan Medical School Ann Arbor, Michigan USA

  2. Outline of lecture • Context of problem- H. pylori • Review relevant gastric physiology • Present ODE model • Present delay and DDE model • Compare results of both • Discussion

  3. Helicobacter pylori (identified in 1982) • Gram negative, spiral-shaped, motile bacteria • Strict human pathogen- colonizes the stomach • Different disease trajectories • Colonization/persistence – superficial gastritis (most common outcome)- acts like IM • Peptic ulcer disease (75% correlated) • Duodenal ulcers (95% correlated) • Lymphomas/ carcinomas • pH-dependent growth, virulence is adherence and motility • Some countries 100% infected, USA:50%, Italy:80% • Treatment: antibiotics for 6 weeks • How does this pathogen survive in the hostile environment of the stomach? • pH, shedding of mucus, sloughing of cells, peristalsis

  4. Introduction to gastric acid secretion • Gastric acid is important for two reasons: • Activation pepsin • Sterilization of the stomach • Maintenance of pH homeostasis is critical for proper function and protection of the stomach. • Gastric acid secretion is diurnal.

  5. Goals • Study how Helicobacter pylori, a strict human stomach pathogen, affects the gastric acid secretion system to allow its infection and persistence • * Develop a virtual human model of gastric acid secretion • *Incorporate a delay to reduce system

  6. The stomach: corpus and antrum regions Corpus Antrum

  7. Gastric glands mucosa mucus gland Taken from H.F. Helander (1992)

  8. Key cell types in the gastric system • Antrum • G cells – secrete Gastrin (+) • D cells – secrete Somatostatin (-) • Corpus • D cells • ECL cells – secrete histamine (+) • Parietal cells – secrete acid

  9. Development of antrum and corpus cells Antrum Corpus

  10. Gastric acid secretion regulation by gastric cells

  11. Gastro-protective mechanisms: bicarbonate secretion

  12. Methods for ODE model system • Developed a system of ordinary differential equations. • Estimated parameters • estimated numbers for each cell population • acquired parameter values from literature with preference given to estimates from human studies • studied the effect of these parameters using sensitivity and uncertainty analyses (latin hypercube sampling/partial rank correlation) • Analyzed the system of differential equations using three approaches: Matlab, Mathematica and code we wrote based on a finite differencing schemes. • Compared simulations results with published experimental data • Performed virtual deletion experiments

  13. Food function profile F(t) Breakfast: 7:00h Lunch: 13:00h Dinner: 19:00h The daily food function profile is representative of the volume of food eaten during each meal. (1 liter maximal volume)

  14. Neural stimulation equations

  15. Cell dynamics: stasis in the short-term

  16. Hormonal dynamics: gastrin, an inducer of gastric acid secretion Taken from Smith et al., 1990.

  17. Hormonal dynamics: somatostatin, an inhibitor of gastric acid secretion Taken from Burhol et al., 1984

  18. Acid dynamics: gastric acid Taken from Feldman and Richardson, 1986.

  19. Hormonal dynamics: histamine, an inducer of gastric acid secretion- no data available

  20. Ion dynamics: bicarbonate, a gastro-protective mechanism

  21. Partial reciprocity of gastrin and somatostatin: positive and negative regulators of gastric acid secretion Taken from Zavros et al, 1999 • Negative Feedback

  22. Stability: attracting limit cycles • A stable period 3- cycle is observed which is a function of food intake

  23. Results of virtual deletion studies • Virtual gastrin deletion study • basal and stimulated acid concentrations are lower than controls during deletion simulations and qualitatively compare with literature (e.g. Wada et al, 1997). • Virtual histamine deletion study • Basal acid concentrations remain normal but stimulated acid levels are drastically reduced during deletion simulations when compared to controls. This results is demonstrated by Kobayashi et al (2000). • Virtual total somatostatin deletion study • Both basal and stimulated gastrin, histamine, and acid levels are increased during deletion simulations when compared to controls. Martinez et al (1998) demonstrate this in studies done in somatostatin deficient mice.

  24. Findings • The system is robust • Cellular and physiological homeostasis observed • Simulation results correlate with experimental data • pH homeostasis is maintained during the course of the virtual experiments • We will now extend the model to assess the interaction dynamics between H. pylori and the virtual host. • Our findings may provide more insight into how H. pylori alters the gastric physiological environment to favor its persistence within its human host.

  25. Discussion • Gastrin is the key regulator of gastric acid secretion • Model is complex, can we reduce? • 18 non-linear ODEs, 1 forcing function • A delay exists between the signals received in the corpus region, and the transference of information to the antrum. • Can we introduce a continuous delay in the system and still capture the qualitative behavior?

  26. Review: stomach anatomy

  27. Continuous Delay functions We explored three different delay functions: • **The total amount of antral gastrin produced in the past minutes; • The average amount of antral gastrin produced in the past minutes; • The percentage of the total amount of antral gastrin produced in the past minutes (p1+p2=1)

  28. Delay physiology • . Amount of gastrin released by G cells in the antrum diffuses gradually into the corpus and is then available to the D and parietal cells only after a certain time period • Thus, the total amount of gastrin released in the previous minutes that is already located in the corpus region is effectively inducing the secretion of somatostatin and acid • This is physiologically relevant as it in part describes the Hill kinetics (i.e., a critical concentration of gastrin is required before a “surge” of its affect is observed)

  29. Figure 2: DDE diagram

  30. Figure 3: ODE vs DDE baseline

  31. Figure 4: phase portraits ODE vs DDE

  32. Figure 5: phase portraits DDE with different delays

  33. Figure 6: Antral Somatostatin depletion

  34. Figure 7: Corpal Somatostatin depletion

  35. Figure 9:Antral Gastrin depletion

  36. Conclusions: • the temporal behavior of the DDE model closely reproduces that of the ODE model • the stability of the ODE system is also observed in the DDE model at a delay length of tau= 30 minutes • virtual depletion experiments further validate that the DDE model replicates the behavior of the ODE system

  37. TheKirschner Lab Brian M. Murphy, PhD David Gammack, PhD Simeone Marino, PhD Suman Ganguli, PhD Ping Ye, MS Seema Bajaria, MS Ian Joseph Benjamin H. Singer Stewart Chang Karyn Sutton Jim Zakowski Christian Ray Vanessa Pherigo Acknowledgments $$ from NIH and The Whitaker Foundation

  38. New equations

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