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Toward Quantitative Simulation of Germinal Center Dynamics Steven Kleinstein stevenk@cs.princeton.edu Dept. of Computer Science Princeton University J.P. Singh J.P. Singh jps@cs.princeton.edu Dept. of Computer Science Princeton University With continual guidance from: Martin Weigert Dept. of Molecular Biology Princeton University Philip E. Seiden IBM Research Center, Dept. of Molecular Biology
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Affinity Maturation (Takahashi et al. J. Exp. Med., 187:885 1998) B cells with affinity-increasing mutations are selected for binding to antigen
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The Germinal Center Physical site of B cell hypermutation and selection http://www.chemistry.ucsc.edu/ Spleen Germinal Center Immunity 1996 4: 241–250
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Experimental studies have elucidated the basic molecular mechanisms underlying the germinal center reaction. (e.g., hypermutation, FDC binding, Apoptosis) However, it is still not well understood how these mechanisms fit together. How does the germinal center work?
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Shortcomings of Current Models Common Models Prototypical Response Qualitative validation Average-case dynamics Mechanism of selection is implicit Our Goal Specific Response Quantitative validation Average & Distribution Mechanism of selection is explicit
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Talk Outline Background Germinal center model during prototypical immune response How to simulate the specific response to oxazolone Experimental validation: average dynamics & individual dynamics Summary & Conclusions
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The Oprea-Perelson Model (Liu et al. Immunity 1996 4: 241) Includes mechanism underlying affinity maturation Oprea, M., and A. Perelson. 1997. J. Immunol. 158:5155. Affinity-Dependent Selection Proliferate & Diversify Dark-Zone Light-Zone Memory Death
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Oprea-Perelson Model Equations Oprea, M., and A. Perelson. 1997. J. Immunol. 158:5155. A complex model that includes many details
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Simulated Germinal Center Dynamics
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Does model apply to specific system? Compare dynamics with data from oxazolone response General Parameters Response Specific Germline Affinity Effect of mutation Half-life Migration Rates Physical Capacity Key Mutations are highly selected in germinal center
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Experimental Validation Step #1 (Berek, Berger and Apel, 1991) The average dynamics of germinal centers
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Experimental Validation Step #2 The dynamics within individual germinal centers (Ziegner, Steinhauser and Berek, 1994) Single Founder (all-or-none) Single Founder (all-or-none)
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A New Implementation is Needed Differential equations implicitly model average-case dynamics and have no notion of individual cells Create new discrete/stochastic simulation of the Oprea-Perelson model Follows individual cells Predicts distribution of behaviors
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Model Differs From Experiment Model predicts 7 founding cells per germinal center
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Limiting the Number of Founders Affinity-Dependent Selection Proliferate & Diversify Decreased Generation (e.g., lower mutation rate) Decreased Selection (e.g. lower probability of recycling) Memory Death Many hypothesis can be tested by changing parameter values
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Affinity Maturation Founders Average Number of Founders R2R2
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Parameter changes alone cannot bring simulation into strict agreement with data on average and individual dynamics simultaneously Two possibilities... Data not correctly interpreted Changes to model are necessary Two possibilities... Data not correctly interpreted Changes to model are necessary
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Is Problem Data Interpretation? The Case for Multiple Founders Can be tested by collecting more data, or stronger statistical tests
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Can Extending the Model Help? Affinity-Dependent Selection Proliferate & Diversify Memory Death Allow selected cells an advantage, independent of affinity Motivation: processes which reduce number of founders restrict the growth rate of the actual founder
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Extended Models Produce Agreement Single founder predicted Extensions can be tested by experiment
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Applied Oprea-Perelson to Oxazolone Allows prediction of specific experiments Quantitative Validation Predicts average GC dynamics Fails to predict individual GC behavior Analysis Two Possibilities Experimental data is not correctly interpreted –Too limited, need to collect more –Develop stronger statistical tests Extensions to OP model are necessary Summary & Conclusions
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