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Transfer Functions for Protein Signal Transduction: Application to a Model of Striatal Neural Plasticity

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  • Gabriele Scheler

Abstract

We present a novel formulation for biochemical reaction networks in the context of protein signal transduction. The model consists of input-output transfer functions, which are derived from differential equations, using stable equilibria. We select a set of “source” species, which are interpreted as input signals. Signals are transmitted to all other species in the system (the “target” species) with a specific delay and with a specific transmission strength. The delay is computed as the maximal reaction time until a stable equilibrium for the target species is reached, in the context of all other reactions in the system. The transmission strength is the concentration change of the target species. The computed input-output transfer functions can be stored in a matrix, fitted with parameters, and even recalled to build dynamical models on the basis of state changes. By separating the temporal and the magnitudinal domain we can greatly simplify the computational model, circumventing typical problems of complex dynamical systems. The transfer function transformation of biochemical reaction systems can be applied to mass-action kinetic models of signal transduction. The paper shows that this approach yields significant novel insights while remaining a fully testable and executable dynamical model for signal transduction. In particular we can deconstruct the complex system into local transfer functions between individual species. As an example, we examine modularity and signal integration using a published model of striatal neural plasticity. The modularizations that emerge correspond to a known biological distinction between calcium-dependent and cAMP-dependent pathways. Remarkably, we found that overall interconnectedness depends on the magnitude of inputs, with higher connectivity at low input concentrations and significant modularization at moderate to high input concentrations. This general result, which directly follows from the properties of individual transfer functions, contradicts notions of ubiquitous complexity by showing input-dependent signal transmission inactivation.

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  • Gabriele Scheler, 2013. "Transfer Functions for Protein Signal Transduction: Application to a Model of Striatal Neural Plasticity," PLOS ONE, Public Library of Science, vol. 8(2), pages 1-13, February.
    • Handle: RePEc:plo:pone00:0055762
    DOI: 10.1371/journal.pone.0055762
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    References listed on IDEAS

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    1. Samuel Bandara & Johannes P Schlöder & Roland Eils & Hans Georg Bock & Tobias Meyer, 2009. "Optimal Experimental Design for Parameter Estimation of a Cell Signaling Model," PLOS Computational Biology, Public Library of Science, vol. 5(11), pages 1-12, November.
    2. Jeremy E Purvis & Ravi Radhakrishnan & Scott L Diamond, 2009. "Steady-State Kinetic Modeling Constrains Cellular Resting States and Dynamic Behavior," PLOS Computational Biology, Public Library of Science, vol. 5(3), pages 1-9, March.
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